Valley of the Moon™ Coffee is the product of our “Boots on the Ground” Valley of the Moon™ Eco Demonstration Project in Panama, www.NaturalSolutionsFoundation.org, where we are helping to reclaim the production of clean, unadulterated food.

Each bag of Valley of the Moon Coffee you give as a gift, or treat yourself to, supports clean food agriculture and supports the Natural Solutions Foundation at the same time. That means that you are drinking clean, toxin-free coffee and supporting health freedom at the same time.

Don’t forget to get yourself some of our exceptional Valley of the Moon™ Coffee, www.ValleyoftheMoonCoffee.org, and remember to give this delightful health brew as your gift for birthdays, Christmas, Hanukkah, corporate gifts, Holiday corporate and private gift giving! Clean, toxin-free coffee helps coffee drinkers, it helps the Natural Solutions Foundation at the same time and it tastes WONDERFUL!!!

In fact, we want you to try, and then keep on drinking, our wonderful Valley of the Moon Coffee™ so we have a coffee special for you: Purchase a 1/2 pound bag of our spectacular coffee for $18.87 plus shipping. This same bag normally requires a donation of $25.00 (a savings of $6.13) plus shipping. Now, purchase 5 bags or more (including your gifts) and your price drops to $17.57 per bag – a savings of $37.15!

Just make sure that you enter “RbR01C” in the Comments Area to receive this special price for Valley of the Moon Coffee, www.ValleyoftheMoonCoffee.org

We need recurring donations so we cover our expenses and plan ahead. Whatever your recurring donation is, it will help to make the difference. We are hacked and attacked for a reason: because we are having an impact.

The other side has huge power. We have more. Together. You see, we have your Push Back power!

The other side has huge budgets. We do not need that much.

The other side deals in lies. We deal in truth. The other side is truly dangerous because they are wreaking havoc and leading people to disease and death.

We are “dangerous” solely because we are telling truth to power.

Thanks for your help. Please take the actions below and please, please make a donation. Your health and food freedom literally depend upon it.

Thanks! Now spend a few minutes disseminating these Action Items to your contacts so they become part of the Incredibly Powerful Mouse Warrior Army!

That’s why our visits to the offices of both incumbents AND candidates, when we come in groups, armed with the talking points, are so very important. That’s why viralizing the Action Items (see above) and the Talking Points (see below) is so very, very, important.

OF COURSE “they” are attacking us! If you were the Uber Cartel and the other side were this successful, wouldn’t you attack them this way if you had no scruples and no desire to see anything like freedom for anyone but yourself?

We can only take this level of attack as a powerful confirmation that we, you and the Natural Solutions Foundation, are exerting a meaningful force against globalization, genocide and the contamination of our food! And that is why we cannot let up!

1. You are interested in finding out more about the Natural Solutions Foundation’s Valley of the Moon™Eco Demonstration Project and how it might fit your needs. You have visited www.NaturalSolutionsFoundation.org and www.MyValleyoftheMoon.org and you are intrigued. Of course, you are welcome at any time but you might want to join Trustee Ralph Fucetola and a group of people for their next visit here (tentative dates: January 19 – 27, 2011). Contact us at dr.laibow@gmail.com, subject PANAMA, for more information.

2. You know that the US is in the process of seizing both IRAs and 401s and “guaranteeing” them with the “strength” of the US Dollar to provide you with an “annuity” of 3% interest and you are not at all happy with this option. You know that you can still place your retirement funds offshore and are seriously considering this option.

3. You want to live in a community of like-minded people with a secure, BeyondOrganic food supply, natural medical center and other services and you want to do it outside the US.

4. You want to help to reclaim the production of clean, unadulterated food around the world through your support of, and connection with, the Valley of the Moon Eco Demonstration Project in Volcan, Panama. You don’t have to be a farmer to do so!

GlaxoSmithKline Agrees to Pay $750 Million to Settle Manufacturing Complaints!

GlaxoSmithKline, the British drug giant, has agreed to pay $750 million to settle criminal and civil complaints that the company for years knowingly sold contaminated baby ointment and an ineffective antidepressant — the latest in growing number of whistle-blower lawsuits that drug makers have settled with multimillion dollar fines. Altogether, GlaxoSmithKline sold 20 drugs with questionable
safety that were made at a huge plant in Puerto Rico that for years was rife with contamination. Cheryl Eckard, the company’s quality manager, asserts in her whistle-blower suit that she warned Glaxo of the problems but the company fired her instead of addressing the issues. Among the drugs affected were Avandia, Bactroban, Coreg, Paxil and Tagamet. No patients are known to have been sickened by the quality problems although such cases would be difficult to trace.

Altogether, GlaxoSmithKline sold 20 drugs with questionable safety that were made at a huge plant in Puerto Rico that for years was rife with contamination. Cheryl Eckard, the company’s quality manager, asserts in her whistle-blower suit that she warned Glaxo of the problems but the company fired her instead of addressing the issues. Among the drugs affected were Avandia, Bactroban, Coreg, Paxil and Tagamet.
No patients are known to have been sickened by the quality problems although such cases would be difficult to trace.http://www.nytimes.com?emc=na

———————————–

FDA Announces Sibutramine Has Been Withdrawn From the Market

The agency asked Abbott Laboratories to pull the drug from the market after it evaluated data from a postmarketing study of the drug’s cardiovascular safety. The study, called the Sibutramine Cardiovascular Outcomes Trial (SCOUT), demonstrated a 16% increase in the risk for serious cardiovascular events such as nonfatal heart attack, nonfatal stroke, the need for resuscitation after the heart stopped, and death in a cohort of patients given sibutramine compared with another given a placebo.
In September, an FDA advisory panel reviewed the SCOUT results, with HALF OF THE MEMBERS IN FAVOR OF WITHDRAWING SUBITRAMINE [emphasis added – REL] and the other half recommending stricter access to the drug and tougher label warnings.http://cme.medscape.com/viewarticle/730515?src=cmemp&uac=117629CN

Note: IF Vaccine$ Worked At All, Why Would 4x Do$e Be Needed? Who $ays It I$ Needed? But It’$ 2x A$ Expen$ive

(NaturalNews) The vaccine industry has now decided that injecting senior citizens with the “standard” vaccine dose just isn’t working. (Gee, really?) So now they’ve decided the way to make it work better is to offer aquadruple viral potency vaccinethat packs 400% more viral fragments into one toxic shot. The target for this quadruple vaccine injection? Senior citizens, of course — the very people most likely to suffer the most serious side effects from a vaccine overdose. The FDA reportedly approved the new vaccine in April even though no scientific tests have ever been done to show it reduces flu symptoms.http://www.naturalnews.com/030164_flu_vaccines_senior_citizens.html

———————————–

Low Testosterone Associated With High Mortality in Men With CHD

October 22, 2010 (Sheffield, United Kingdom) — Among men who have coronary heart disease, mortality was doubled in those with low testosterone levels compared with those who had normal levels, a new observational study has shown. Dr Chris J Malkin (Royal Hallamshire Hospital, Sheffield, UK) and colleagues report their findings in Heart. [1]

“This is the fourth epidemiologic study to have shown that low testosterone is a marker of early mortality,” senior author Dr Kevin S Channer (Royal Hallamshire Hospital, Sheffield, UK) told heartwire . “But most crucially, it is the first in men with vascular disease; all of the other epidemiologic follow-up studies of testosterone have excluded this patient population.” http://www.medscape.com/viewarticle/731060?sssdmh=dm1.644521&src=nldne&uac=117629CN

Natural Solutions Foundation: Note, however, that when cholesterol is artificially lowered, the sex hormones, including testosterone, cannot be produced in adequate supply. Heart disease is “treated” by lowering cholesterol to ultra low, non-physiologic levels with statins. Subsequent conditions like depression, erectile dysfunction, stroke, cancer, heart attacks and death are likely results. Bad medicine, good business. REL

A good friend of health freedom wrote to Diane Feinstein (D CA) about his flu vaccine concerns. He received the predictable form letter containing such idiocy as “Several studies have been conducted, by the CDC and other agencies, in response to concerns that thimerosal, a mercury-containing component of the influenza vaccine, is linked to autism. These studies did not find such a link, noting that the amount of thimerosal in the vaccine was too low to have an effect. One study found that, even after thimerosal was removed from vaccines in Denmark, the rate of autism in children continued to rise.

The influenza vaccine is the safest, most effective method of preventing the spread of a disease which, according to the CDC, leads to an average of 36,000 deaths each year. Please know that I will keep your thoughts in mind should legislation regarding the influenza vaccine come before the Senate.

Sincerely yours,
Dianne Feinstein
United States Senator”

Our articulate friend wrote back to her a letter which I now share with you with thanks to him for his activism, his passion and his sharing of this exchange.

“Dear Diane,

Thank you so much for your email regarding the use of the deadly mercury in the H1N1 vaccine and other injections given even to newborn babies with no regard to the long term neurological consequences and the damage that will be done to millions of families across our country and around the world. I appreciate your need to do all you can for the reputation of the WTO, after their complete exposure as a fraudulent organization when they issued a pandemic alert of the highest level last year (level 6) in order to convince (or coerce) millions of people to take the toxic vaccines.

I sympathize with you that the otherwise well-coordinated scam did not work, and the “pandemic” had to be canceled, with millions of unused injections sitting on the shelves, waiting for a pandemic to be created fast enough to use them before they have to be thrown away. No one realizes how hard the poor drug dealers work with their government servants to pull off one of these global scams, and how much hard-extorted money they lose when one does not work. Actually, though, since the government bought the injectable drugs from them, there is fortunately no loss to the drug dealers themselves, but only to the American public, since this was a taxpayer expense.

As far as your reassurance that CDC and FDA have made sure these toxins are really good and healthy for us to inject into our bodies, thank you that makes me feel so much better. I realize that as a busy senator, you have no spare time to waste on things like learning what the CDC and the FDA are, or that they are fully controlled by and take their orders from, the drug companies. Later, when you are retired, perhaps you can take the time to study these things, instead of just repeating what you have been told. If you eventually become honest, and perhaps develop a conscience, you will find that the current “health care” system, overseen and controlled by the respectable drug lords that you know as “pharmaceutical companies” has become the number two cause of death in American today (something like 750,000 deaths a year from “properly” used drugs).

I look forward to the time you become interested in what good you could actually do for the people you are supposed to represent. There is still time for you to drop the party and political nonsense, and take up humility, honesty, and a sincere interest in truth instead. Millions of us are waiting for that time and wishing you well in getting there.

In the meantime, if you ever develop any curiosity to see the real data on vaccines, take a look at:

www.homefirst.com, and www.healthfreedomusa.org, and numerous others which are not connected to the vast “health care” drug machine. The information is rock solid, science based, and will amaze you if you allow yourself to learn.

European Food Supplements Directive, which we have described as “Codex on steroids” is set to go into full implementation in April, 2011. In our rapidly globalizing world, does this spell the end of high potency nutrients and supplements in the US? Find out this coming Sunday at 10 AM – 1 PM Eastern

To Listen or Ask Questions Call: 512-904-8014 or Toll Free 866-841-1065(If www.HealthFreedomPortal.org is down, we have an alternative program link at www.DrRima.net)And on November 7th… You are invitee to join our
Round Table Discussion of the election and
How the results will effect health and food freedom issues…
We will have some surprise guests then too!

And remember to supplement with Cognitive Enhancement Nutrients to keep your brain healthy and focused…this message from our friends at Biologics Nutraceuticals, providers of the Cognitive Enhancement Nutrition:

“Please let Health Freedom supporters know they can take advantage of our Double Dip Sale with $4.99 Economy Shipping to the entire US! All of the Dr. Rima Packs are discounted 10% with the additional option to buy 2 and get another pack of the same type added to your cart at checkout for free! You may also buy three of the same type individual bottles and receive a free bottle of the same type in your cart at checkout!” Brian

Valley of the Moon™ Coffee is the product of our “Boots on the Ground” Valley of the Moon™ Eco Demonstration Project in Panama, www.NaturalSolutionsFoundation.org, where we are helping to reclaim the production of clean, unadulterated food.

Each bag of Valley of the Moon Coffee you give as a gift, or treat yourself to, supports clean food agriculture and supports the Natural Solutions Foundation at the same time. That means that you are drinking clean, toxin-free coffee and supporting health freedom at the same time.

Don’t forget to get yourself some of our exceptional Valley of the Moon(TM) Coffee, www.ValleyoftheMoonCoffee.org, and remember to give this delightful health brew as your gift for birthdays, Christmas, Hanukkah, corporate gifts, Holiday corporate and private gift giving! Clean, toxin-free coffee helps coffee drinkers, it helps the Natural Solutions Foundation at the same time and it tastes WONDERFUL!!!

In fact, we want you to try, and then keep on drinking, our wonderful Valley of the Moon Coffee™ so we have a coffee special for you: Purchase a 1/2 pound bag of our spectacular coffee for $18.87 plus shipping. This same bag normally requires a donation of $25.00 (a savings of $6.13) plus shipping. Now, purchase 5 bags or more (including your gifts) and your price drops to $17.57 per bag – a savings of $37.15!

Just make sure that you enter “RbR01C” in the Comments Area to receive this special price for Valley of the Moon Coffee, www.ValleyoftheMoonCoffee.org

WE ARE BEING SERIOUSLY HACKED AND ATTACKED – AGAIN!

WHY? BECAUSE OUR PUSHBACK IS WORKING AND THE POWERS THAT BE ARE NOT AMUSED!“We are NOT Amused!”

This is the second time I have written this blast tonight. When I pushed “Save” a few moments ago, the whole blast disappeared. Is that an attack? I don’t know, but keep reading to find out what the indisputable attacks look like today alone:

Here’s what Patrick, our computer guy, wrote to me in today’s report about why our links are not working and we can’t log in to our sites – and, often, neither can you:

“1. Fake donations are logged into the site which we have to spend time and effort sorting out from the real ones, and which we have to pay for as bad charges. Two years ago, this cost us over $10,000 when our bank account was invaded and the “charges” taken from from our account.
2. We have several problems with our sites ‘going missing’, meaning that one day we have the site and the links work correctly but the next day we don’t. See below to understand more of how that is happening.
3. Our Site Hosting was changed against our will and without our knowledge or permission
4. All Security Logs and Access Records were cleaned out, as in ‘the archives were wiped out’. These archive are our security records of who has accessed the site, which means that all of the records of who went into what file and did what to it – are now gone.
5. The Password to our main hosting and domain service was changed without our knowledge or wish
6. Someone changed all our name servers so that the site would not display properly.

While it is possible that this was merely the result of a poor setup, I don’t think this was an accident. We use the services of several different companies and all of them have been attacked in the ways I am describing. The items that were changed would have to have been done by someone with access to our systems, and with knowledge of who else we had web services through.” [Note from General Stubblebine: not necessarily: if the incursion is at a high level, there is no need to assume that someone knows our passwords and therefore can do this sort of damage. In fact, if NSA or high-level corporate espionage is involved, this type of incursion would be very, very easy for them.]
Patrick goes on to say, “Note: By ‘Web Services’ I mean Hosting, Domain Names, File Storage, Email, and the like.
7. The Healthfreedomusa.org site, on which I have been working, was hacked OR Cracked. There was no major damage done, that I can tell, but there was damage. Several files were deleted, some pictures, and some links were messed up making it harder for us to get products to the people who order them and to help people navigate to our other pages. These incursions are nothing that can’t be fixed, but are a definite time, money, and energy drain.”

Why is this happening? Because we are winning and the other side is running scared. That’s why our nearly 800,000 emails on S. 510, S. 3767 and GMOs to the Senate are so important.

Clean Phude? Phude Safety? Give the FDA more power so they can “protect” us? Take a look at what they are doing with the power they already have and ask yourself if giving an agency that says IN COURT that you do NOT have a right to eat food you want MORE power is OK. If not, then taking action against S. 510 and S. 3767 are imperatives for you.

“In the thirty years of Morningland Dairy operations NO ONE has become ill from consuming their products. Yet they have been ordered by the Missouri Milk Board to destroy ALL of their cheese without actual tests being performed on the cheese stock. This is nearly 50,000 pounds of cheese, or approximately $250,000.
Since the Milk Board and the FDA showed up at Morningland on August 26th, they have been “embargoed” from shipping or making any product. They dumped their milk for nearly six weeks before being approved to send it into homogenized, pasteurized distribution. All the while, they have had to pay the bill to keep the dairy and cheese plant operational….”

That’s why our visits to their offices when we come in groups, armed with the talking points, are so very important. That’s why viralizing the Action Items (see above) and the Talking Points (see below) is so very, very, important.

OF COURSE they are attacking us! If you were the Uber Cartel and the other side were this successful, wouldn’t you attack them this way if you had no scruples and no desire to see anything like freedom for anyone but yourself?

We can only take this level of attack as a powerful confirmation that we, you and the Natural Solutions Foundation, are exerting a meaningful force against globalization, genocide and the contamination of our food! And that is why we cannot let up!

Yesterday I was a guest for 3 hours on the Mike Chambers Show. Literally every time I began to speak in-dept about the intentional contamination of the US food supply and the genocidal underbelly of this plan, or about vaccinations and their part in the genocide, the connection was lost and Mike was on the show by himself. Listen here, http://www.oraclebroadcasting.com/archives.php?stream=/midnightrider/midnightrider.2010-10-13_16k.mp3, to decide for yourself if it was random or regulated. Much the same thing happens in our Dr. Rima Reports show every Sunday morning from 10 Eastern Time to 1 PM at www.OracleBroadcasting.com or to listen with live chat, www.HealthFreedomPortal.org.

When we talk with Mark Lerner, a leading advocate against the Real ID biometric version of state intrusion this Sunday, October 17, we’ll see if the same thing happens!

Frankly, Let’s Be Clear About Something:

The Natural Solutions Foundation cannot operate without your support. Right now, half way through the month of October we do not have enough funds to go to the Codex Committee on Nutrition and Foods for Special Dietary Uses meeting in Chile early in November. What that means is that you will be, where Codex is concerned, blind and deaf. Your eyes and your ears, Gen. Bert and I, will not be there bringing you the real scoop, not some watered down, balsaamic happy nonsense. But to get there, we need your support. Now.

There are a number of reasons, all of them good ones, that I can think of.
Here are some of them, in no particular rank order:

1. You are interested in finding out more about the Natural Solutions Foundation’s Valley of the Moon™Eco Demonstration Project and how it might fit your needs. You have visited www.NaturalSolutionsFoundation.org and www.MyValleyoftheMoon.org and you are intrigued. Of course, you are welcome at any time but you might want to join Trustee Ralph Fucetola and a group of people for their next visit here (tentative dates: January 19 – 27, 2011). Contact us at dr.laibow@gmail.com, subject PANAMA, for more information.

2. You know that the US is in the process of seizing both IRAs and 401s and “guaranteeing” them with the “strength” of the US Dollar to provide you with an “annuity” of 3% interest and you are not at all happy with this option. You know that you can still place your retirement funds offshore and are seriously considering this option.

3. You want to live in a community of like-minded people with a secure, BeyondOrganic food supply, natural medical center and other services and you want to do it outside the US.

4. You want to help to reclaim the production of clean, unadulterated food around the world through your support of, and connection with, the Valley of the Moon Eco Demonstration Project in Volcan, Panama. You don’t have to be a farmer to do so!

5. You want to attend our outstanding seminars and workshops, like Angela Malek’s “Living, Eating and Healing with the 5 Element Theory” Workshop from January 9 – 15, 2011. Watch a short video with Angela here: http://www.youtube.com/watch?v=RKmOB6VdctQ to get the “flavor”. Interested? Contact us at dr.laibow@gmail.com with “5 Elements” as your subject line. More information: http://drrimatruthreports.com/?p=7035 — Space is strictly limited!

6. You love good food and the idea of reclaiming its production. You love eating it, too, and you can’t wait to eat at our gourmet organic restaurant!

7. You want to volunteer your time and talents at the Valley of the Moon! Again, use our dr.laibow@gmail.com address with “Volunteer” in the subject line.

The Supreme Court is grappling with the question of how much protection the 1986 National Childhood Vaccine Injury Act was meant to provide vaccine manufacturers against lawsuits. The case involves Hannah Bruesewitz, whose parents claim that a Wyeth-manufactured D.T.P. vaccine she received as an infant in 1992 led to developmental problems. At issue is whether Bruesewitz’s parents should be allowed to sue Wyeth on the premise that the drug maker could have offered a safer vaccine but opted not to do so. The case has moved from the “vaccine court” to the Pennsylvania state court to federal court; Wyeth has thus far prevailed.

Actelion Pharma Failed To Report 3,500 Deaths

The same FDA which has chosen to believe that more than 3500 in utero deaths following H1N1 vaccination, up from 7 potentially flu-related spontaneous abortions in an average year, is insignificant and therefore does not constitute a significant increase worthy of safety responses, says that 3500 unreported deaths by Actelion Pharma IS significant. Noting that doctors under report drug and vaccine reactions by about 97%, the agency says “we do not agree that a determination of a relationship between Traceable use and death by 3 percent of healthcare providers who did respond to Actelion is insignificant. And the agency adds that there is no suggestion that healthcare providers “who did not respond to Actelion did not also believe there was…a relationship” between death in individual cases.

October 14, 2010 — Data from industry-sponsored trials published in peer review journals are misleading the public about the safety and efficacy of their drugs, according to 2 reports published online October 13 in the British Medical Journal (BMJ).

In a meta-analysis that looked at all of the published and unpublished data on the antidepressant reboxetine (Pfizer) for the short-term treatment of major depression, investigators concluded that the drug was not only ineffective but also potentially harmful.

They also report that 74% of the data on patients who took part in the trials of reboxetine were not published because the findings were negative and that the data that were published about reboxetine overestimated its benefits and underestimated its harm.

“This meta-analysis provides a striking example of publication bias, in which the previously favourable risk-benefit profile of reboxetine shown in published trials is reversed by the addition of unpublished data,” Beate Wieseler, MD, deputy head of the Department of Drug Assessment at the Institute for Quality and Efficiency in Health Care, Cologne, Germany, told Medscape Medical News.

We’re getting ready to return to Federal Court for the next round of the Stop the Shot Case. Last year your Push Back stopped mandated vaccines and the planned Swine Flu pandemic; your support let us go to Federal Court to challenge the FDA’s approval of the “novel” virus, but unsafety-tested, vaccine and the states that were mandating the vaccines backed off.

This year the Swine Flu virus has been added to the seasonal flu vaccine and we’re heading back to court. This year’s Complaint is stronger than last year and challenges ALL influenza vaccines. But to make it to court we must raise substantially more funding.

To donate, please go to http://drrimatruthreports.com/?page_id=189#StS

And supplementing with Cognitive Enhancement Nutrients to keep your brain healthy and focused… this message from our friends at Biologics Nutraceuticals, providers of the Cognitive Enhancement Nutrition:

“Please let Health Freedom supporters know they can take advantage of our Double Dip Sale with $4.99 Economy Shipping to the entire US! All of the Dr. Rima Packs are discounted 10% with the additional option to buy 2 and get another pack of the same type added to your cart at checkout for free! You may also buy three of the same type individual bottles and receive a free bottle of the same type in your cart at checkout!”

Support the Natural Solutions Foundation’s “Stop the Shot” Federal Lawsuit to prevent the use of any influenza vaccine. Set up a recurring donation now:http://drrimatruthreports.com/?page_id=189
This long, detailed and immensely important article makes it crystal clear where the lies and distortions are about vaccines, whether they work, whether they cause chronic illnesses and whether they are safe.

Before you allow yourself or your wards, children, family, elders or others to take another vaccination, read this article. Listen to Dr. King discuss this article on the Dr. Rima Reports live (www.HealthFreedomPortal.org to join the chat and listen to the show or at www.OracleBroadcasting.com to listen to the show or in the archives at www.OracleBroadcasting.com following the broadcast on Sunday, October 3, 2010, 10 AM to 1 PM Eastern time.

Dr. King knows full well that vaccines are intentionally used to create disease and profit while they do nothing to prevent disease. Listen to him, read the article below and share this article as widely as possible.
Thanks for your activism.Yours in health and freedom,
Dr. Rima

Introduction
Before discussing the subjects in the title of this article, this commenter would be remiss if
he did not first set forth his biases and conflicts concerning the issues discussed in the sections and
paragraphs that follow this introduction.
As a scientist who understands that:
? Terms must be clearly defined,
? Statements must be supported by factual evidence and, where that evidence is not
readily available, appropriate citations thereto,
? Much of the information on vaccines and vaccination programs available in the
mainstream media and publications backed by the Establishment and its minions is
more propaganda, cant and Orwellian newspeak than sound science, and
? Vaccines or vaccination programs where the vaccine is reasonably safe and the
protection provided is either life saving (e.g., the rabies vaccines) or the prophylactic
vaccine is reasonably safe and effective in protecting almost all (i.e., >90 %) of those
vaccinated, long-lasting (i.e., protects that not less than 90 % of those vaccinated for
a period of not less than 50 years), and medically cost-effective, for example, the
measles only vaccine and vaccination program) should be supported,
this commenter must stand against: a) the misrepresentation of vaccines and vaccination programs
in any manner, and b) vaccination programs in which: i) those inoculated with the vaccine are not
protected or ii) more who are vaccinated suffer serious adverse injury from the vaccine than there
are disease cases in the population segments that are being vaccinated (e.g., the early childhood
hepatitis B vaccination program).
In addition, since the Establishment continually spews out a never-ending stream of near-
religious vaccine and vaccination apologia, this author sees no need to spend any time discussing
the inflated and often deceptive presentation of vaccines and vaccination programs as the
“salvation” of mankind – because such discussions belong in the realm of religion and not science.
With the preceding in mind, this author will now begin to address fundamental vaccine and
vaccination-program misrepresentations that stand in the way of our right to choose or decline any
prophylactic medical treatment, including any prophylactic inoculation with any vaccine or serum
as we, and not society, sees fit for ourselves and the minors and non-competent persons in our care.

1. “Vaccines Are Safe”

The first misrepresentation about vaccines and by far the worst is that, as a group (or
individually), “vaccines are the safest of medicines” or, more simplistically, “vaccines are safe”.
The factual evidence and the legislation protecting the vaccine makers, vaccine providers

1
Where the term “knowing” is used in the “knowingly” or “knew” sense that is defined in 21 U.S.C. § 321(bb) “The
term “knowingly” or “knew” means that a person, with respect to information – (1) has actual knowledge of the
information, or (2) acts in deliberate ignorance or reckless disregard of the truth or falsity of the information”.
and the healthcare establishment clearly exposes a different reality, which, in its most telling form,
can be found in the National Vaccine Injury Compensation Program (NVICP2; Title 42 of the
United States Code in Sections 300aa-10 through 300aa-34 [42 U.S.C. § 300aa-10 – 300aa-34]) in §
300aa-22(b)(1) which, under: a) the umbrella of “Standards of Responsibility” (§ 300aa-22.) and b)
the heading at § 300aa-22(b), “Unavoidable adverse side effects; warnings”, states:
“No vaccine manufacturer shall be liable in a civil action for damages arising from a
vaccine-related injury or death associated with the administration of a vaccine after
October 1, 1988, if the injury or death resulted from side effects that were unavoidable even
though the vaccine was properly prepared and was accompanied by proper directions and
warnings”. [Emphasis added]
If vaccines were truly safe, then there would be no need for: a) any NVICP legislation to
protect the vaccine makers or the healthcare providers from civil lawsuits for damages, or b) any “if
the injury or death resulted from side effects that were unavoidable” language to absolve vaccine
manufacturers from damages that include “vaccine-related injury or death”.
Clearly, unbiased scientists, the federal lawmakers, and the informed public know that, as a
group or, in most instances, individually, vaccines are not the safest medicines.

2. “Vaccines Are Effective”

If vaccines were truly effective, then there would be:
a. No need for any State to mandate any vaccination program for any vaccine –
everyone would be demanding inoculations for themselves and their loved ones,
b. No need for any mention of the unproven theory of “herd immunity”, which, in
reality, can only be a theory of “herd protection” because vaccines do not provide
blanket immunity (defined as lifetime [>50 year] protection from disease) to even
those who have been inoculated with the recommended vaccines from 2 to 6 or more
times, depending upon the vaccine, and
c. No need to license vaccines based on their manufacturers’ claimed levels of
“efficacy” as measured by some minimum-antibody-level surrogate for
effectiveness.
Given the preceding factual realities, it is clear to any rational person that unqualified
phrases, like “vaccines are safe” and “vaccination programs are effective”, are simply propaganda
slogans that vaccine makers, the healthcare establishment, pro-vaccine academics, pro-vaccine US
governmental agencies (e.g., Department of Health and Human Services [DHHS], the Centers for
Disease Control and Prevention [CDC], the Food and Drug Administration [FDA], the National
Institutes of Health [NIH] and the Public Health Service [PHS], to name a few) and other vaccine
apologists continually use in their efforts to both brainwash and coerce the public into accepting
whatever vaccines and vaccination programs that “these groups” have decided, at a given point in
time, are “good” for the public as a whole with little or no regard for the fiscal or physical health of

2
The full title of the NVICP in the United States Code is: TITLE 42 – THE PUBLIC HEALTH AND
WELFARE, CHAPTER 6A – PUBLIC HEALTH SERVICE, SUBCHAPTER XIX – VACCINES, Part 2 –
National Vaccine Injury Compensation Program.
any individual or individuals that such vaccination programs may harm, maim or kill or, for that
matter, the fiscal and physical health of the people of the United States Of America (USA).

3. “Vaccine Panacea: The More Vaccines We Get, The Healthier We Will Be”

a. The Legacy (Pre-NVICP) Vaccination Programs
Reviewing the history of vaccines and vaccination programs in the USA, up until the early
1900s, the only widely used human prophylactic (disease-preventive) vaccine was the live-virus
cowpox vaccine, vaccina; the only other general human-use vaccine was the attenuated rabies
vaccine used to treat people who had been bitten by a rabid animal; and the only large-scale mass
“vaccination” program was the “smallpox” inoculation program.
In the 1920s, a diphtheria vaccine was introduced and its use spread; in the 1950s, the use of
pertussis vaccines became widespread but these morphed into the first combination the DTP
vaccine, which was to become the first Thimerosal-preserved combination vaccine to be used in a
mass vaccination program.
In the 1950s, the Salk inactivated-polio vaccines were introduced for mass use without
adequate testing and purity leading to: a) an initial increase in paralytic polio cases until the clinical
definition of paralytic polio was changed and b) the introduction of SV-40 and other animal viruses
which were, to varying degrees and levels, contaminants of all the polio vaccines produced for the
next three decades; and, a few years later in the early 1960s, the live-virus Sabin oral polio vaccines
displaced the Salk inactivated-polio vaccines – the Sabin oral polio vaccines were used in the USA
until 2000 when, because all paralytic polio cases were cases caused by exposure to the vaccine-
strains of the live vaccine, the US switched back to a Salk-type inactivated-virus polio vaccines,
which is still in use today.
In 1963, a live-virus measles vaccine was introduced and put into mass use shortly after its
introduction; the measles-only vaccine was followed by a measles-rubella (Merck’s measles-rubella
vaccines, MR® and MR® II, that have been discontinued); then a measles-mumps-rubella vaccine
(Merck’s MMR® vaccine); and finally an improved measles-mumps-rubella vaccine (Merck’s
MMR® II vaccine)3.
In the early 1980s, though some other vaccines were being licensed, they were not being
recommended for mass use in childhood vaccination programs because of the increasing number of
lawsuits where the parents of vaccine-injured children, principally by the DTP vaccines and the
Polio vaccines but also by the measles and MMR vaccines, were winning ever larger monetary
judgments against the vaccine companies.
Faced with decreasing profit from the lawsuits, the major vaccine makers threatened to stop
making vaccines unless the government passed legislation that protected them from most all direct
civil legal actions for the harm their vaccines caused in some of the children who were being
inoculated with these vaccines.

3
In addition to the combination measles-mumps-rubella vaccines (MMR® and then MMR® II), Merck continued to
make the individual component vaccines, Attenuvax®, Mumpsvac®, and Meruvax® II until the mid-2000s. In 2010,
Merck announced that, in spite of customer demand for the individual vaccines, Merck would not resume
producing these vaccines.
3
from the pen of Paul G. King, PhD
In late 1986, comprehensive legislation was enacted that included the National Vaccine
Injury Compensation Program (NVICP) that was codified in 42 U.S.C. §§ 300aa-10 through 300aa-
34 and, in stages, became effective in 1987 and 1988.
This legislation was originally supposed to: a) provide a speedy, “no fault”, non-litigious,
fair compensation program for vaccine-injured children and their families, which, after initial
appropriations to start the program, was to be paid for by a tax on each disease component in each
dose of vaccine administered, and b) shield the vaccine makers from being easily sued.
In return for this protection, the vaccine manufacturers were supposed to make ever-safer
vaccines that caused less adverse reactions under strict governmental oversight that would not only
compel vaccine makers to make safer vaccines but punish them when they did not make vaccines as
safe as possible and reduce the risk of adverse reactions.
In actuality, all that the NVICP has done is shield the vaccine makers from being sued and,
through an increasingly slow, litigious, convoluted, and unfairly administered “compensation
program”, its administrative hearings have only compensated a very small percentage of those who
are damaged by adverse reactions to vaccines even though the program has been expanded to
include adults in many instances.
In 1987, Congress took the first action to decrease the fairness of the program and reduce the
financial burden on the federal government and the vaccine makers for any violation by repealing §
300aa-18, which indexed the compensation for both vaccine-related death and the vaccine
manufacturers’ fines to the rate of inflation.
Next, the NVICP program administrators started making it harder for children’s families to
collect for vaccine injuries by, in the 1990s, removing many of the indications from the “Vaccine
Injury Table” (see: Sec. 300aa-14. Vaccine Injury Table) without any independent scientifically
sound justification for removing them, which forced many more cases to be heard in a proceeding
that has become increasingly litigious and unfair4.
In the late 1980s, though it was clear that the diphtheria, tetanus, acellular pertussis (DTaP)
vaccines produced a lower rate of adverse reactions in children given them than the corresponding
diphtheria, tetanus, whole-cell pertussis (DTwP) vaccine, based on the data from Japan, which
introduced the DTaP vaccine in 1981 and saw a sharp decline in both diphtheria-tetanus-pertussis-
vaccine-related adverse reactions and vaccine-related deaths, the DTwP vaccines were still licensed
and being given in the USA until 1997, when the vaccine makers finally switched to making the
DTaP vaccine5.

4
This continual indication reduction process has gone beyond the absurd, removing the rotavirus vaccine indication
for intussusception even though all of the rotaviruses have been shown to cause intussusception in some vaccinated
children and two new rotaviruses (a 5-component bovine-human hybrid rotavirus vaccine [RotaTeq®] and an
attenuated human rotavirus vaccine [Rotarix®]) have been licensed and approved for mass use instead of amending
the table entry for the withdrawn RotaShield ® rhesus-monkey/human hybrid rotavirus vaccine and, most recently,
proposing to further alter the allowable time windows for the few remaining indications in the Vaccine Injury Table
(see: Federal Register / Vol. 75, No. 176 / Monday, September 13, 2010 / Proposed Rules / 55503 – 55507).
5
As one article correctly reports, “4) The old whole-cell version of DPT, given until about 1997 in the US, was bad. It
had a high rate of serious reactions, and these researchers calculated its effectiveness at only around 48%. But for the
previous 20 years, parents in the US were being told their children must have this vaccine. The real truth about a

After all, after 1986, the vaccine maker’s principal goad to make safer vaccines, the
monetary awards to successful plaintiffs in civil court cases seeking compensation for the injuries
caused by their vaccines, had been removed.
By comparison, the legal replacement for this goad was a weak and obviously ineffectual
federal governmental bureaucracy over which the vaccine makers obviously had significant
influence, and, given Merck’s Gardasil HPV vaccines’ problems and the federal government’s
failure to take any substantial action against the vaccine or the vaccine maker, currently have even
greater influence.
b. The NVICP and Post-NVICP Vaccination Programs
With the passage of the NVICP legislation, the stream of vaccines from a growing number
of vaccine makers and/or their subsidiaries has increased to a veritable river.
Discarding any semblance of a need for cost-effectiveness in any mass vaccination program,
the Establishment has moved to not only add more doses of vaccines that were already marginally
cost-effective or not even cost effective but also to propagandize vaccination programs where the
underlying vaccine is not even truly effective or, in some cases, not even reasonably safe.
In addition, the Establishment, using a hired Institute of Medicine (IOM) committee as its
surrogate, redefined the allowable “placebo” in a vaccine clinical safety trial from only a pH-
buffered sterile isotonic saline solution to include: a) the entire vaccine formulation without the
active antigens, b) some other experimental vaccine or c) some other licensed vaccine, and
convinced the regulators to look at relative incidence of adverse events instead of their absolute
incidence in determining that a given vaccine is “reasonably safe”.
Together, these changes altered the basis for “safety” in phase 3 clinical trials and, by
increasing the adverse reactions in the “placebo” group, reduced the relative level of each adverse
reaction in the candidate vaccine compared to that adverse reaction in the “placebo” group.
Thus, when “three” children in the test group for Merck’s RotaTeq® vaccine in as clinical
trial (conducted in an overall population where sanitation is poor) developed intussusception and
“one” child in the control group developed intussusception, the RotaTeq vaccine was still
approvable and approved because the rate of intussusception was not significantly higher (on a
statistical basis) than the rate in the controls because of the small size of the groups in phase 3 trial
that Merck had conducted.
On this basis, the FDA licensed Merck’s genetically engineered, bovine-human-hybridized,
pentavalent, oral, live-virus rotavirus vaccine, RotaTeq, even though this vaccine’s actual rate of
intussusception was 3 times that found in the control group.
Of course, after its approval in February of 2006, the pediatricians were told that, unlike the
previous “intussusception prone” rotavirus vaccine, Wyeth’s RotaShield®, which was withdrawn
shortly after its introduction in 1998, RotaTeq’s on-label use would not cause intussusception.
Even after being told that RotaTeq does not cause intussusception, the RotaTeq-related
intussusception signal in the voluntary Vaccine Adverse-Event Reporting System (VAERS) [where

particular vaccine being kind of dangerous and ineffective doesn’t come out until the pharmaceuticals decide they
have something better” (emphasis added). [See: http://www.exploringvaccines.com/?p=686]
typically less than 10% of actual adverse events for a given vaccine are reported] was even larger
after RotaTeq began to be used than the signal seen from the previous, now-withdrawn
“intussusception prone” RotaShield rotavirus vaccine and, in addition, RotaTeq-related cases of
Kawasaki’s disease were also reported6.
Additionally, after the NVICP was enacted, several patently unsafe or problematic vaccines
were licensed (e.g., LymeRX™ for Lyme disease and RotaShield® for rotavirus) and, after causing
horrendous or significant harm to those vaccinated with them from which the Establishment
profited, simply withdrawn from the market.
Thus, in addition to the pre-NVICP childhood vaccination programs for DTP, MMR and
Polio, we now have ineffective and/or less-than-effective vaccines and less-than-effective and/or
non-cost-effective mass vaccination programs for: a) late-childhood/adult diphtheria-pertussis-
tetanus (Tdap), b) childhood Haemophilus influenzae, type B (Hib), c) early childhood/adult
Hepatitis B (Hep B), d) childhood chickenpox, e) childhood/adult Hepatitis A (Hep A), f)
childhood/adult meningococcal meningitis (Sanofi Pasteur’s Menomune® and Menactra® vaccines),
g) Streptococcus pneumoniae (Wyeth’s Prevnar® and Prevnar ® 13[childhood] and Merck’s 23-
valent Pneumovax® [adult]), h) childhood rotavirus (Merck’s RotaTeq® and GlaxoSmithKline’s
(GSK’s Rotarix®), i) adult Shingles, and j) mid-childhood/young-adult human papilloma virus
(HPV; Merck’s Gardasil® and GSK’s Cevarix®) as well as k) ineffective annual vaccines and
annual vaccination programs for viral influenza in children and adults with “11” different vaccine
formulations currently being produced in “eight” manufacturing sites.
Moreover, not only does this require more and more vaccines to be given during childhood
but also, further unmasking the reality that vaccination is not immunization, to increase “coverage”
(in reality, market size and market penetration), adults are increasingly recommended to: a) get
“boosters” doses or “booster” vaccines, b) get periodic Tdap boosters in lieu of tetanus boosters,
and c) accept additional vaccine doses whenever there is a disease outbreak of a “vaccine
preventable” disease in their community regardless of their disease status.
In addition, no meaningful action has been taken against the vaccine makers for their failure
to expeditiously safen US vaccines by removing all preservatives and reducing the level of
adjuvants used or, where possible, eliminating the use of adjuvants altogether.
Instead, though there currently is a limit on the permitted level of aluminum adjuvant in
each vaccine7, the total level of aluminum adjuvants administered is being allowed to increase
without limit and the vaccine makers are increasingly demanding that they be permitted to use so-
called “oil-in-water” adjuvant systems even though, based on animal usage, these are known to be
more serious immune-system disruptors than the current long-used aluminum adjuvants whose
long-term safety for use in human vaccines has not been proven individually much less collectively.

6
Geier DA, King PG, Sykes LK, Geier MR RotaTeq vaccine adverse events and policy considerations. Med Sci
Monit. 2008 Mar; 14(3): PH9-PH16.
7
If the FDA’s proposed changes to 21 CFR § 610.15. Requirements for constituent material as published in the
Federal Register (see: Federal Register 2010 March 30; 75(60): 15639-15642) are adopted by the FDA, the FDA
will be able to waive all of the current limits, including those for preservatives and adjuvants as it sees fit even
though doing so is a subversion of the foundation upon which the regulation o all drugs is based – the applicable
regulations as set forth in 21 CFR Parts 600-680 are current good manufacturing practice (CGMP) minimums,
which every covered biological drug product must meet.

Finally, in spite of being sued for the failure of the Secretary of the Department of Health
and Human Services (hereinafter, the Secretary) to make vaccines safer and reduce the risk of
adverse reactions, as required by 42 U.S.C. § 300aa-27(a), by removing Thimerosal (49.55 %
mercury by weight) from the list of approved chemicals that can be used to manufacture vaccine,
the federal government has yet to ban the use of Thimerosal, a chemical that is known to induce
anaphylactic shock in some and mercury poison susceptible developing children, in the manufacture
of vaccines.
c. The Number of Vaccine ‘Doses’ Reality
Increasingly the public is being told that they must submit to ever-expanding vaccination
programs for themselves and their children without regard for the risks to their own health or the
health of their children because complying is for the “greater good”.
For children up to 6 years of age, the recommended vaccination program reached a new high
in 2009 when, in addition to all of the 38 vaccines in the 2007 and 2008 vaccination programs, three
more doses of an 2009-A-H1N1 influenza vaccine was added for a nominal total of 41 doses of
vaccines.
Relative to 1983, the maximum relative level of mercury from possibly Thimerosal-
preserved vaccines (marked in red in Table 1 on the next page) was 1.6 times the nominal level of
exposure in 1983 and, roughly correcting for 10-or-more-times-larger effect of the prenatal
mercury dose, effectively up to 5-plus times the level of adverse impact relative to the vaccine
exposure to injected Thimerosal (49.55% mercury by weight) in 1983.
d. The Continuing Use of Mercury (Thimerosal, 49.55% Mercury by Weight) Reality
When it comes to the issues surrounding the serious adverse health impacts of Thimerosal
(49.55% mercury by weight) on those vaccinated with vaccines containing it, the public is
continually propagandized with one of two misleading and inaccurate slogans:
1. “Mercury has been removed from all childhood vaccines” or
2. “All vaccines given to children, except some flu vaccines, no longer contain any added
mercury”.
The reality is that the Establishment, faced with a growing public outcry against the use of
Thimerosal as a preservative in childhood vaccines, did gradually reduce the level of Thimerosal in
the previously Thimerosal-preserved vaccines from nominally 25 micrograms of mercury per 0.5-
mL dose to about 1 mcg of mercury per 0.5-mL dose (a reduced-Thimerosal or “trace”-Thimerosal
vaccine formulation) in the period from 2001 to 2005 and then starting in 2004, phased out the use
of Thimerosal in childhood vaccines.
However, to offset this reduction in mercury exposure from childhood vaccines (and the
serum Rho(D) products), the Establishment-controlled CDC began publishing recommendations in
April of 2002 that, during the annual flu season: a) pregnant women who would be in their second
and third trimesters and b) children 6 months to 23 months of age should get a flu shot (see
Prevention and Control of Influenza Recommendations of the Advisory Committee on
Immunization Practices [ACIP]. MMWR 2002 April 12; 51(RR03): 1-31) at a time when all FDA-
approved influenza vaccines were Thimerosal-preserved vaccines.

4 through 6 years DTP (48) MMR (48) MMR (48)
OPV (48) DTaP (48) DTaP (48)
[2; 10] IPV (48) IPV (48)
Varicella (48-60) Varicella (48-60)
[25; 125 mcg Hg] Influenza (54) Influenza (54)
Influenza (66) Influenza (66)
[6; 38] [6; 41]
[50; 150 mcg Hg] [50; 200 mcg Hg]
Vaccines and values in a red font are for vaccines that were, in 1983, or, in the 2000s, may still
be, Thimerosal-preserved.
The CDC made these recommendations in spite of the fact that the flu vaccines were
“Pregnancy Category C” vaccines with no proof:
a. Of non-teratogenicity for the fetus or reproductive safety for the pregnant women;
b. That the flu vaccines were not mutagenic or carcinogenic; or
c. That the flu vaccines were in-use effective in preventing those vaccinated from
contracting influenza.
There was, as is the case today, also no proof that flu vaccines, of any kind, are more in-use
effective than a placebo injection in preventing those children under 2 years of age who are
inoculated with a flu vaccine from contracting influenza.
As: 1) the level in the childhood vaccines continued to declined, 2) some doses of “trace”-
Thimerosal flu vaccines became available, and c) a live-virus flu vaccine was introduced, the CDC
recommendations continued to try to maintain the adverse effects of the average level of mercury
exposure to Thimerosal by: a) removing the restriction as to when, during pregnancy in the flu
season, flu shots could be given; b) increasing the upper limit on children to first 35 months, then to
59 months, then to 107 months, and, finally, to 18 years of age; and c) requiring children to get two
flu shots (a month apart) the first time they were vaccinated.
In 2009, the maximum level of Thimerosal exposure was doubled in utero and at 6 months
and 7 months when the CDC: a) added the “pandemic”, “swine flu”, 2009-A-H1N1 influenza to the
vaccines recommended to be given once to pregnant women and twice to children under 9 years of
age, and b) also designated pregnant women and young children as targeted “high risk” groups.
Since:
? Most of the doses of available influenza vaccines are Thimerosal-preserved doses,
? The CDC steadfastly refuses to even express a preference for pregnant women and
young children to get “no Thimerosal” influenza vaccine doses and
? The FDA continues to illegally license Thimerosal-preserved vaccines for which the
vaccine manufacturer has never proven that the level of Thimerosal used as a
preservative in said inactivated-influenza vaccines is “sufficiently nontoxic …” as
required by the applicable portion of the current good manufacturing practice
(CGMP) safety regulations set forth in 21 CFR § 610.15(a),
pregnant women and children are continuing to be injected with toxic levels of mercury from
these adulterated drugs8
Moreover, given the CDC’s decision to increase the upper age limit for children to 18 years
and recommend that all adults be vaccinated annually, if Thimerosal-preserved flu shots continue to
be administered and some children and their mothers during pregnancy only get Thimerosal-
preserved flu shots, clearly the total dose of mercury exposure will continue to exceed the
maximum level that children born in the 1990s would have received from the three Thimerosal-
preserved childhood vaccines, DTaP, Hib, and Hep B, given to all children before 2001 and to some

8
Thimerosal-preserved vaccines for which the manufacturer has failed to meet the applicable clear CGMP minimum
“sufficiently nontoxic …” requirement for the vaccine dose set forth in 21 CFR § 610.15(a) are adulterated drugs
under 21 U.S.C. § 351(a)(2)(B).
9
from the pen of Paul G. King, PhD
children into the 2004 – 2005 timeframe, if no changes had been made to the Thimerosal-preserved
childhood vaccines or in the recommendations for the use of Thimerosal-preserved inactivated-
influenza vaccine formulations to inoculate pregnant women and developing children.
As long as the preceding realities continue to exist, any claim that there can be no link
between: a) the level of mercury exposure and b) the risk of neurodevelopmental disorders, chronic
illnesses and abnormal behaviors is obviously a specious claim because the maximum level of
mercury has not dropped from the 2000 level but rather the maximum exposure level has increased.
At the same time, the levels of neurodevelopmental disorders, chronic medical conditions,
and abnormal behaviors have not dropped but rather these levels have also collectively increased.
Based on the preceding and other key facts (e.g., the several-fold excess level of males as
compared to females in the neurodevelopmental disorders and the fact that increases in these
disorders were noticed a couple of years after the 3-dose regimens for Thimerosal-preserved Hep B
and for Hib were implemented in the late 1980s in the USA and in the 2000s after similar program
changes were implemented in New Delhi, India9), this author knows that mercury exposure from
Thimerosal in vaccines and other drugs is the major causative factor in many, if not all, of the
epidemic-level increases in neurodevelopmental disorders, chronic medical conditions, and
abnormal behaviors.

4. “The Benefits Outweigh The Risks”

Pointing to our current increased life expectancies and ignoring their projected future
decline, the Establishment continually tells Americans that the benefits of each new vaccination
program outweigh the risks.
Unfortunately, there has been epidemic increases in many chronic diseases (e.g., asthma in
children from < 1 in 1,000 children in the 1970s to > 1 in 10 children in the 2000s) and the
morphing of previous chronic diseases only seen in adults (e.g., type 2 diabetes) into chronic
diseases seen in children to the point that, in 2006, more than 26 % of American children have one
or more chronic diseases (up from 12.8 % in 1994)10 that they most probably will have over their
lifetime.
Thus, the “greater good” for whom each of us is supposed to sacrifice ourselves and our
loved ones is, in actuality, the “greater good” for one or more segments of an Establishment that
feeds on us and grows ever stronger as more of us weaken and become chronically ill and/or
financially and physically drained trying to care for our chronically ill loved ones.
Worse, there is increasing evidence that those who are effectively in control of this
Establishment decided have, unconsciously or consciously, that they need to:

9
The reality of this linkage was recently strongly reinforced by the emergence of a similar pattern’s being observed
in a New Delhi, India nursery school after the New Delhi pediatricians began recommending the addition of 3-
doses each Thimerosal-preserved Hib and Hep B vaccination programs to the Indian government’s recommended
Thimerosal-preserved DTP vaccination program in 2000 and the worsening of the outcomes when these programs,
originally designed to finish the 9-shot vaccination series by the time the children are 6 months of age, were
shortened to be completed by 4.5 months of age and the incidence of neurodevelopmental dysfunction doubled.
[See: http://dr-king.com/docs/100711_ParallelsinNewDelhiIndia_AnEpidemic_b.pdf.]
10
Van Cleave J, Gortmaker SL, Perrin JM. Dynamics of Obesity and Chronic Health Conditions Among Children
and Youth. JAMA 2010 February 17; 303(7): 623-630.
? Increase the harm,
? Further drain our fiscal and physical strength, and
? Reduce our numbers and our life expectancy, while feeding on our fiscal and physical
strength.
To that end, increasingly expensive vaccines (e.g., Merck’s Gardasil and GSK’s Cervarix,
where the private-sector list price for each dose is than US $125.0011) that: a) are less-and-less
curative and/or effective and b) seem to be more-and-more harmful are being approved and
delivered to the public as preventives for conditions whose incidence, in many instances, may have
been caused or aggravated by other vaccines, drugs, processed and genetically altered foods, and
chemicals that the Establishment markets to the public as “safe” without any real proofs of the
short-term and, more importantly, true long-term safety for any of these Establishment products.
To sell these less-than-effective, less-than-proven-safe, and much-more-expensive vaccines,
the Establishment continually reminds the public of the horrors of the deaths from “vaccine-
preventable disease” for certain highly contagious and lethal diseases from the era before vaccines
(e.g., smallpox, polio and measles), diseases that have disappeared (e.g., smallpox) or only occur at
low levels (e.g., measles) in the USA today, while ignoring or minimizing the following critical
realities:
? Clean water, sanitation, basic food safety, improved housing, and antibiotics did
more to reduce the level of the disease-related injuries and fatalities from the highly
contagious and lethal diseases than the vaccines for them have done,
? Without any vaccine, scarlet fever, a highly contagious and lethal disease, has
virtually disappeared
? Many of today’s vaccines are for diseases that: a) are not highly contagious (e.g.,
influenza and hepatitis B) or b) do not have any significant mortality levels (e.g.,
chickenpox, mumps, rubella, and tetanus).
? The obviously vaccine-related increases in chronic diseases, especially chronic
diseases that have a significant autoimmune component, like asthma, multiple
sclerosis, chronic fatigue syndrome, lupus, and diabetes, to name a few, as well as
epidemic increases in abnormal childhood neurodevelopment, abnormal behaviors,
other developmental abnormalities and bowel disorders.
In addition, when we were first being sold on mass vaccination programs as a means to
protect the health of the public, we were told that a mass vaccination program for any vaccine
depended on the vaccine’s being effective and the mass vaccination program’s being cost effective.
Consider the “chickenpox” vaccination program where the vaccine, Merck’s Varivax®, is a
live-virus vaccine that infects every one inoculated with it with a certain strain, the Oka/Merck
strain, of herpes varicella zoster (HVZ) – a vaccine strain that is not effective in preventing

11
CDC Vaccine Price List (Prices last reviewed/updated: September 24, 2010): Merck’s HPV-Quadrivalent (Types 6,
11, 16 and 18) Recombinant Vaccine, Gardasil, US$ 130.27/dose; GSK’s HPV-Bivalent (Types 16 and 18)
Recombinant Vaccine, Cervarix, $ 128.75/dose, where both process include a US$ 0.75 excise tax nominally
collected for the NVICP in 10-dose vials: $1302.70 plus shipping and handling for each Gardasil vial and $1287.50
vial. The commercial list price costs of the two 3-dose series are US$ 390.81 and US$ 386.25, respectively.
11
from the pen of Paul G. King, PhD
everyone vaccinated, or even all of those with a “sufficient” vaccine-strain antibody titer level, from
also being infected by the “native”/“wild” strains of HVZ circulating in the USA.
When the initial licensing for this vaccine was sought in the 1990s, the justification for
licensing a chickenpox vaccine for a normally mild and innocuous childhood disease was that
vaccination was marginally cost-effectiveness on a societal productivity-loss basis under the
presumptions that: a) one dose of vaccine would provide lifetime protection for most young
children inoculated with the vaccine and b) there would be no serious adverse reactions to being
inoculated with the vaccine.
Yet, today, two doses of Varivax® are the minimum recommended for all children, and older
adults are being recommended to receive a dose of Merck’s Zostavax®, a higher-concentration Oka-
strain HVZ vaccine to “prevent” a recurrence of the HVZ (native or vaccine-strain) with which they
have been infected.
Without even considering the costs to treat those who have severe adverse reactions to the
Varivax or Zostavax vaccines, a conservative 2009 cost analysis placed the US excess shingles’
cases’ costs, caused by the US childhood chickenpox vaccination program, at US$ 700 million
annually.
Clearly, the Establishment has discarded the requirements for vaccine effectiveness and
vaccination-program cost-effectiveness.
In their place, Establishment profitability seems to have: a) overruled the federal
government’s concern for public’s fiscal and physical health and b) trumped the significant costs
from the collective long-term vaccination-induced physical harm, including maiming and death,
that some of those who are vaccinated suffer12 when the serious adverse effects caused by the initial
vaccine, Varivax® (which was claimed to cause no serious adverse effects in the FDA-
licensing/approval process), Merck’s MMR-Varicella vaccine, ProQuad® (which has a significantly
higher risk of serious adverse effects), and Merck’s shingles HVZ vaccine, Zostavax®, are factored
in.
Currently, the Establishment is engaged in introducing vaccines, like Merck’s Gardasil® and
GlaxoSmithKline’s Cervarix®, with no proof of long-term effectiveness and self-generated, self-
serving “cost effectiveness”, which clearly ignore the costs to those who have had, are having and
will have serious adverse reactions
Furthermore, after their approval, the CDC immediately recommended mass vaccination
programs for these vaccines with almost no in-use proof of safety and no in-use proof of
effectiveness in preventing cervical cancer.
Worse, both the CDC and the FDA seem almost total indifferent to the hundreds of reported
vaccine-induced injuries as well as the tens of vaccine-linked deaths, which, quite predictably, the
Establishment attributes to mere coincidence.
In addition, the Establishment has introduced vaccines, like the current rotavirus vaccines,
that have clearly negative US cost-effectiveness (where the cost of the vaccination program far

12
Tellingly, before Merck’s Gardasil® HPV vaccine was introduced, Varivax consistently had the highest incidence
of adverse-event reports in the VAERS database in the 1990s and early 2000s.
exceeds the costs of the background level of rotavirus in the USA) and, for Merck’s genetically
engineered RotaTeq®, have clearly increased US rotavirus disease risk in those children and adults
who were previously “immune” to the native human rotavirus strains to which they have been
exposed during their childhood but are not protected from being infected by the genetically
engineered bovine-human hybridized viruses in Rotateq.
Moreover, the standards for licensing a vaccine in the USA have been reduced from the
vaccine: a) must be truly effective in preventing the disease in most of those who have been
vaccinated and b) must reduce the harm from the disease in those who are vaccinated and still
contract the disease as well as c) reduce the transmission of the disease to:
? In the case of the rotavirus vaccines, for the limited and biased clinical trials
conducted, the vaccines were approved based on a finding that the risk of the serious
harm caused by the vaccines is not statistically higher than the risk of harm caused
by the natural disease in the control population used in the phase-3 clinical trials.
? In the case of the human papilloma virus (HPV) vaccines, the vaccines were
approved based on claims that the vaccines may, in this instance, prevent some
vaccine-associated cervical cancers in some of the vaccinated women three to five
decades after they complete the initial 3-dose vaccination schedule, even though:
a. There is no proof that HPV infection causes cervical cancer — only proof that
HPV infection levels are associated with cervical cancer,
b. The “efficacy” data indicates a post-vaccination loss of efficacy in less than a
decade,
c. The strains of HPV in either vaccine (HPV types 6, 11, 16, and 18 in Gardasil
and types 16 and 18) are not even the major strains of the disease prevalent in
the USA – in fact the type 11 strain is almost non-existent (“0.1%”) in the US
women13, and
d. The approvals are not questioned when the levels of adverse-event reports,
including serious maiming and death, currently far exceeds the level of the
other vaccines even though only a small percentage of the eligible population is
being vaccinated with these vaccines while the level of vaccination in most of

13
Dunne EF, Unger ER, Sternberg M, McQuillan G, Swan DC, Patel SS, Markowitz LE. Prevalence of HPV
Infection Among Females in the United States. JAMA. 2007 February 28; 297(8): 813-819.
“RESULTS
The most common HPV types detected were HPV-62 (3.3%; 95% CI, 2.2%-5.1%) and HPV-84 (3.3%; 95% CI, 2.2%-
5.1%), HPV-53 (2.8%; 95% CI, 2.1%-3.7%), and HPV-89 (2.4%; 95% CI, 1.4%-4.3%) and HPV-61 (2.4%; 95% CI,
1.6%-3.8%) (FIGURE 2). HPV-16 was detected in 1.5% (95% CI, 0.9%-2.6%) of females aged 14 to 59 years. There
was no statistically significant difference in the prevalence of HPV-16 and the 13 more commonly detected types, except
for HPV-84 and HPV-62. HPV-6 was detected in 1.3% (95% CI, 0.8%-2.3%), HPV-11 in 0.1% (95% CI, 0.0 %-0.3%;
relative SE_30%), and HPV-18 in 0.8% (95% CI, 0.4%-1.5%) of female participants. Most participants infected with
HPV (60.1%) had only 1 HPV type detected (95% CI, 53.2%-67.9%); however, 23.9% had 2 types (95% CI, 18.3%-
31.3%) and 16% had 3 or more types detected (95% CI, 12.0%-21.2%). Overall, HPV types 6, 11, 16, or 18 were
detected in 3.4% of the study participants, corresponding with 3.1 million females with prevalent infection with HPV
types included in the quadrivalent HPV vaccine. Few participants (0.10%) had both HPV types 16 and 18 and none had
all 4 HPV vaccine types. At least 1 of these 4 HPV types was detected in 6.2% (95% CI, 3.8%-10.3%) of females aged
14 to 19 years.”
“CONCLUSION
… Our data indicate that the burden of prevalent HPV infection among women was higher than previous estimates.
However, the prevalence of HPV vaccine types was relatively low”. [Emphasis added.]
the other vaccine programs that generate significant levels of serious adverse
events generally exceed 75 % of the population segments covered by the
vaccines.
5. “The Establishment’s Efforts To Increase Their Protection From Civil Lawsuits Are
Appropriate”
Furthermore, through an appeal in Bruesewitz v. Wyeth being heard by the US Supreme
Court this Fall, the vaccine makers and the rest of the Establishment are essentially attempting to
have the Supreme Court rule that the 7th Amendment14 of the Constitution of the United States of
America, an integral part of the “Bill of Rights” reserved to the people of the United States of
America, does not apply to those who have suffered, or are the guardians of those who have
suffered, a vaccine-induced injury.
The artifice being used to carry this argument is that 42 U.S.C. § 300aa-22. Standards of
responsibility is an issue that can be decided once, and for all, by the judiciary, outside of a civil
trial by jury on the facts of each case.
This argument is being advanced even though, under the NVICP, the vaccine maker’s lack
of liability under § 300aa-22 is supposed to be the issue decided in the first phase of any vaccine-
related civil jury trial.
That such liability decisions belong to the trial jury is clearly set forth in § 300aa-23. Trial,
which at § 300aa-23(b), states:
“(b) Liability
The first stage of such a civil action shall be held to determine if a vaccine
manufacturer is liable under section 300aa-22 of this title”. [Emphasis added.]
Moreover, the Establishment’s arguments knowingly ignore § 300aa-22(b) with respect
“warnings”, in general, and § 300aa-22(b)(2), which states:
“For purposes of paragraph (1), a vaccine shall be presumed to be accompanied by proper
directions and warnings if the vaccine manufacturer shows that it complied in all
material respects with all requirements under the Federal Food, Drug, and Cosmetic
Act [21 U.S.C. 301 et seq.] and section 262 of this title (including regulations issued
under such provisions) applicable to the vaccine and related to vaccine-related injury
or death for which the civil action was brought unless the plaintiff shows – …”
[Emphasis added.]
Since:
? As the putative causative DTP vaccine in question is a Thimerosal-preserved vaccine
given to the child and
? The vaccine manufacturers have admitted knowingly failing to comply with Title 21
of the Code of Federal Regulations (21 CFR) as set forth in section 610.15(a) (21
CFR § 610.15(a)), which requires the level of preservative must be proven to be

14
“In Suits at common law, where the value in controversy shall exceed twenty dollars, the right of trial by jury shall
be preserved, and no fact tried by a jury, shall be otherwise re-examined in any Court of the United States, than
according to the rules of the common law”.
“sufficiently nontoxic so that the amount present in the recommended dose of the
product will not be toxic to the recipient”, in testimony given before a Congressional
committee which investigated the vaccine makers and the US Food and Drug
Administration’ actions from 1999 and which subsequently published a formal
Congressional report, “Mercury in Medicine – Taking Unnecessary Risks” in 200315
and the requirement in question is a material requirement under the Federal Food,
Drug, and Cosmetic Act [21 U.S.C. 301 et seq.] as well as a safety regulation issued
under the provisions in “section 262 of this title”16 [emphasis added],
the Wyeth defendant is clearly guilty of failing to comply “in all material respects with all
requirements under the Federal Food, Drug, and Cosmetic Act [21 U.S.C. 301 et seq.] and section
262 of this title (including regulations issued under such provisions) applicable to the vaccine and
related to vaccine-related injury or death for which the civil action was brought”.
Moreover, recognizing defendant Wyeth’s knowing and intentional failure to comply with
the black letter law, the US Supreme Court should, when it hears the case this Fall: a) find for the
Bruesewitz plaintiffs and b) take whatever actions needed to ensure that the Bruesewitz plaintiffs
are awarded appropriate punitive damages for defendant Wyeth’s knowing and willful failure to
comply with 21 CFR § 610.15(a) for the preservative Thimerosal in the vaccine that caused the
harm to the Bruesewitz child.
However, given the Establishment’s denial of reality of vaccine-induced mercury toxicity in
susceptible children, like the Bruesewitz child, who were, and are still being, given vaccines
preserved with Thimerosal (49.55% mercury by weight) and the power that the Establishment
wields, the people will be lucky if the US Supreme Court finds for the Bruesewitz plaintiffs.
Finally, should the US Supreme Court find for Wyeth, then, the people will most assuredly
know that both the Establishment and the US Supreme Court are knowingly severing those who
bring vaccine cases against the vaccine manufacturers in the legal manner provided by NVICP from
the right to a civil jury trial for damages that is supposedly guaranteed by the 7th Amendment to the
Constitution of the USA.
6. “The ‘Life Saving’ Annual Influenza Vaccination Program”

Factually, there is no scientific proof that the influenza vaccine prevents even most (> 50%)
of those who are “vaccinated” with an influenza vaccine from contracting and spreading influenza
during the “flu season” – none whatsoever (see, for example, Geier DA, King PG, Geier MR.
Influenza Vaccine: Review of Effectiveness of the U.S. Immunization Program, and Policy
Considerations. J. Am. Physicians and Surgeons 2006 Fall; 11: 69-74 [the only US-population-

15
See Finding 3, “3. Manufacturers of vaccines and thimerosal, (an ethylmercury compound used in vaccines), have never
conducted adequate testing on the safety of thimerosal. The FDA has never required manufacturers to conduct adequate safety
testing on thimerosal and ethylmercury compounds” (page 6), in May 2003, Subcommittee on Human Rights &
Wellness of the Government Reform Committee, US House of Representatives (Chairman Dan Burton – following
a 3 year congressional investigation), “Mercury in Medicine – Taking Unnecessary Risks” pgs 1-80 and, in
abbreviated form, published in the Extended Congressional Record: Subcommittee on Human Rights and Wellness,
Committee on Government Reform of the House of Representatives, “Mercury in Medicine Report,” Washington,
DC, as published in the Congressional Record, pgs. E1011-E1030, May 21, 2003
16
Here, “this title” is “TITLE 42 – THE PUBLIC HEALTH AND WELFARE” of the United States Code.
wide retrospective of in-use effectiveness evaluation – not model – for the influenza vaccination
programs in the USA for the years 1979 through 2001]); and other unbiased independent studies as
well as the independent reviews of the published studies (see, for example: Jefferson T, Di
Pietrantonj C, Rivetti A, Bawazeer GA, Al-Ansary LA, Ferroni E. Vaccines for preventing
influenza in healthy adults. Cochrane Database of Systematic Reviews 2010, Issue 7. Art. No.:
CD001269), which clearly show that the inoculation of populations with influenza vaccines, both
inactivated- and, more recently, live-virus, is not effective in preventing those who are inoculated
from getting “influenza” during the “flu season”.
Furthermore, there is some evidence that getting an influenza inoculation in one year may
increase the inoculated individual’s risk of contracting an influenza infection in a subsequent year
(http://www.ageofautism.com/2010/05/with-flu-season-over-canada-shows-flu-vaccinations-to-be-
worse-than-worthless-.html).
Additionally, a recent double-blind clinical trial study found that supplementation with
vitamin D-3 was much more effective in preventing influenza-type-A infections than influenza
vaccination (see: Urashima M, Segawa T, Okazaki M, Kurihara M, Wada Y, Ida H. Randomized
trial of vitamin D supplementation to prevent seasonal influenza A in schoolchildren. Am J Clin
Nutr. 2010 May; 91(5): 1255-1260. Epub 2010 Mar 10. PMID: 20219962).
Finally, as is usually the case, Establishment’s fear mongering and propagandizing carefully
hides the fact that influenza is not a highly contagious disease (see: Cannell JJ, Zasloff M, Garland
CF, Scragg R, Giovannucci E. On the epidemiology of influenza. Virol J. 2008 Feb 25; 5: 29 [Note:
Among the issues this electronically published review article addresses is the absence of any valid value for the sick-to-well infectivity for human influenza in spite of numerous attempts to determine even a valid estimate, which clearly establishes that influenza is not highly infective.]).
Thus, the Establishment is recommending mandates for various groups of people, and the
State of New Jersey is currently mandating, a non-effective vaccination program for a disease that is
not highly contagious on the grounds that, to say the least, this less-than-scientifically-sound, non-
effective prophylactic treatment, influenza vaccination, will somehow protect those who submit to it
from spreading a disease that it does not prevent them from contracting, and, when those inoculated
get the live-virus vaccine, a disease with which those receiving it not only are directly infected by
three strains of live viral influenza but have also been shown to shed the live virus for at least 21
days after being inoculated with said live-virus vaccine.
Furthermore, in spite of an ever-increasing body of evidence that vitamin D-3
supplementation is a more effective preventive for type “A” influenza than any influenza vaccine,
this Establishment continues to ignoring this proven and highly effective prophylactic use of
vitamin D-3, which protects all against contracting all strains of type “A” human influenza, instead
of suboptimal protection from getting the two (2) type A strains of flu in the flu vaccine.
Obviously, the Establishment’s recommendations and actions are not grounded in sound
science nor based on public health concerns; they are clearly driven by other imperatives.
7. “Medical Mandates Are Required For The ‘Greater Good’”

Whenever this author hears any group or zealot, including any vaccine apologist,
recommending that any person should surrender his or her right to make his or her own informed
medical decisions to some “higher authority” (be it employer, state or nation) “for the greater
good”, this commenter knows that the group or person advocating for such is a medical fascist17
who is seeking to take away our personal freedom to make medical choices for ourselves and those
for whom we are responsible and who is advocating for a “religious cult”, the cult of the “public
health” vaccinationists, who seek to mandate that all must sacrifice or risk sacrificing some aspect
of their own or their children’s health on the vaccine altar “for the greater good” – the good of the
Establishment – of which the group or individual demanding the surrender of the rights to informed
choice and consent is a well-paid member, who depends on promoting these sacrifices for his or her
status, position, and/or livelihood.
8. “Vaccines, the Safest of Prophylactic Healthcare Measures”

We are repeatedly sold the myth that “vaccines are the safest disease-preventive medicines”,
when the truth is that, as a group, they are the least safe of disease-preventive medicines (see: Neil
Z. Miller’s Vaccine Safety Manual For Concerned Families and Health Practitioners, 2nd
edition (2010), ISBN 978-188121737-4) and the only class of prophylactic medicines for which
there are no long-term safety studies and, increasingly, not true-placebo-controlled short-term large-
scale safety studies (in a vaccinated versus totally unvaccinated [using sterile isotonic pH-balanced
saline for the controls] with > 50,000 in each arm of the study).
In addition, instead of proof of effectiveness and long-term (lifetime [> 50-year protection])
effectiveness, we are given antibody-titer-based measures of claimed efficacy of limited duration
(typically, 10 years or less) for “most vaccines” after typically 2 to 5 inoculations for most
(typically, > 60%) of those who are initially inoculated multiple times, with a carefully concealed
reality that each such inoculation campaign kills a few18 who are inoculated and harms some
additional multiple of that number each year to varying degrees.

9. “Vaccines Do Not Cause Autism Or Any Other Chronic Medical Condition”
How much longer will Americans tolerate the increasingly obvious lie that the
Establishment’s vaccination programs are not a causal factor in ‘Autism’ and other chronic
childhood medical conditions that once were rare (< 1 to 2 instances in every 10,000 children) but
are now at epidemic levels (> 1 instance in every 10 to 1,000 children)?
How much longer will the American public continue to tolerate the epidemics of chronic
diseases; and epidemic rates of chronic disease that, for asthma, now exceed 10 % of our children
and, in the aggregate, have brought us to a nation where, in 2006, more than 25%19 of our children
have at least one chronic lifetime medical condition so that the Establishment may continue to grow

17
Defined here as any member of medical community who favors dictatorial medicine where all medical decisions
are under the control of the “medical police” and “medical courts”; and the individual has no rights to make his or
her own informed medical decisions without fear of any retribution, ostracism or oppression.
18
Based on the reality that vaccination accounts for most of our excess infant mortality rate over that infant mortality
rate in Japan in the first year of life, this “few” deaths per vaccination collectively translates to about 2 per 1,000
live births or about 8,000 – 9,000 newborn babies in the USA each year.
19
“The rate of chronic health conditions among children in the United States increased from 12.8% in 1994 to 26.6%
in 2006”. [http://www.medscape.com/viewarticle/717030?sssdmh=dm1.591574&src=nldne&uac=140083MY] [Note: 26.8/12.8 is about a
factor of 2.1 – without considering the increase in population of children by about 50% – making the population
percentage increase not 210 % but rather 300+ %.]
18
and profit at the expense of the increasing damage to the fiscal and physical health of ourselves and
our children?
How much longer will the American public be blinded by the propaganda spewed forth
daily by these servants of greed who have been and are knowingly sacrificing our health and
prosperity so that the Establishment they serve may continue to grow in size and profit while our
fiscal and physical health is stolen from us?
Even though this commenter cannot answer for those who read these questions, his past and
on-going efforts clearly point out the reality that he has lost his tolerance for the status quo and, with
eyes wide open, he is seeking to open the eyes of the public to the preceding realities and to march
with that informed and enlightened public to change the USA, not for the “greater good”, but rather
for a return to a system of laws in which the rights of every competent citizen are respected and
everyone has the freedom to freely choose, or reject, all prophylactic vaccination programs without
any penalty, stigma, or recriminations from those who do not share the same views.
In addition, this commenter is: 1) seeking to change the laws protecting the Establishment’s
vaccine purveyors from being held directly accountable for the harm their vaccine products cause
and the lack of safety and/or appropriate effectiveness of many of their vaccine products and 2)
hoping that, after reading this commentary, those who ‘get it’ will join with this commenter in
demanding: a) direct vaccine purveyor accountability and b) the absolute right to choose which, if
any, vaccination programs and when, if ever, the vaccines chosen should be administered – or,
simply, “opt in” vaccination laws in every State, which would repeal the current mandates and
eliminate any and all need for an exemption of any type from any prophylactic or other vaccination
mandate.

About Paul G. King, PhD
Paul G. King, PhD Analytical Chemist, is a scientist who has studied both vaccines and
vaccination programs intensively for more than a decade and has sorted out the underlying science
to the extent that he could find such from all of the published information available from those with
differing views about vaccination and vaccination programs.
If any, after reading this article, any reader finds any significant error for which there is
unbiased science that clearly supports your alternative views, then, by all means, send your
alternative view or views and their supporting documentation to me through dr-king@gti.net and, if
your studies are truly unbiased, this author will be glad to: a) modify his views accordingly and b)
publish an updated article. If you find areas where the text has grammatical, spelling or word-
usage errors, please let the author know so that he may appropriately correct them and published a
revised version of this article.
For additional information about Dr. King and his interests, the reader can visit his
personal web site, http://www.dr-king.com/.

Half of All FDA Approved Drugs are Quietly Withdrawn Within 5 Years of Approval

“FDA approved” drugs means “safe”, right? Clinical trials show that drugs and vaccines are safe or they wouldn’t be allowed to be marketed, right? Drug companies have to report what actually happens in a clinical trial, right? Once a drug is approved by the FDA for market release it stays available for a long time, right?
Lethal and potentially lethal side effects from FDA approved drugs are rare, right?

The answer to these questions is one big collective, “NO!!!!!”

Here are the facts: Drug companies are free to suppress negative clinical trial information with impunity. That is not how the system is designed to work, at least on paper, but it is the way things work in the real world.

Drugs, all drugs and vaccines, enter Phase IV clinical trials when they are released for general use. Depending on how many people they kill, maim, blind or cause to suffer once doctors start prescribing the drug for whatever the FDA has approved it for, although they can use the drug for anything they want to (called “off label prescribing”). Even the callous, corrupt and conflict-of-interest-riddled FDA withdraws approximately 50% of all approved drugs within 5 years of approval because they are just too toxic to continue on the market.

How did they get approved in the first place? Well, as you will see when you read the articles below, drug companies disregard the requirements to be honest in reporting data as they choose. Given that it can cost up to a billion dollars (yes, you read that right, a billion US dollars) to research a drug and bring it to market, there is an enormous amount of pressure to get the drug into the patients’ hands by putting it in the doctor’s mind and getting it onto his/her prescription pad – no matter what.

One of the may ways drug companies accomplish what they want – drug sales, is to lie about how many people die or drop out in drug trials.

Another way is by literally purchasing the decision-makers for stock options, research grants and other inducements plucked fresh from the abundant and ever self-replenishing FDA Corruption Tree.

The results? Pharmaceutical Mayhem.Drugs are the leading cause of death in the US and every other “developed” nation. But, not to worry, the FDA is on the job.! Oh, good. I was worried there for a moment!

You know, insultingly enough, the FDA expects you to believe that these deadly drugs released to the public to see what happens (and what happens is mayhem and murder much of the time) could possibly be an accident? Neither do I. Remember, these same drug companies are big players at Codex. They are the heirs and legatees of the German genocidalists who created Codex Alimentarius, now degrading the world’s food supply as a stepping side to “the Great Culling”, the death of 90% of the world’s population.

Bottom line, from where I stand? If you are not in an Emergency Room, there is, in my experience and belief, no reason to take drugs when inexpensive, gentle, effective and powerful natural options exist through orthomolecular medicine, homeopathy, naturopathy, chiropractic, acupuncture, Bio Acoustics, NeuroBioFeedback, Frequency Medicine, chelation, detoxification and a host of other helpful, safe techniques await your decision-making. But that is the very point, isn’t it? If you are an immensely powerful drug company and you know that your drugs are toxic, expensive, dangerous, poorly conceived and poorly tested, grossly dishonestly marketed what would you do? Jeopardize your cash bonus and tell the truth, wasting a billion bucks? Probably not. Probably you would do what the drug companies (and the BioTech companies which make GMOs and are usually one and the same as the drug companies!). You would lie, and lie big!
“These drugs are safe.” “The clinical trials show it.” “People do not get sick from our drugs.” “We followed the rules.” “You can trust us!”

“The study started out with 20 subjects…For about a week there were 14 subjects. Then they started dropping…Now, we’re down to 7.”
Below, a testimonial by Ana Cantu who was one of the healthy volunteers –“a human guinea pig” as she describes herself– in a month long study that tested the effects of Norvir, an HIV drug made by Abbott Laboratories, when coupled with the antidepressant Wellbutrin, made by GlaxoSmithKline.”

Her first-hand experience provides insight about the immense “pressure for positive results in clinical trials,” the level of discomfort a human subject is expected to endure from the adverse effects of the tested drug (or combination of drugs), and the dilemma for drug manufacturers whose drug causes adverse effects so severe, the test subjects in pre-marketing trials drop out in droves. The FDA accepts study results–even if only 7 of 20 subjects complete the study. Companies are loathe to scrap a negative study: they hold on to the last 7 subjects despite severe adverse effects. The “volunteers” suffer for the payment which they would forfeit if they quit.
Ana describes how and why corporate sponsors–in her case, GSK and Abbott Labs–conceal adverse event data that may damage a drug’s chances for approval.

Despite federal law requiring companies to fully disclose to the FDA all adverse events in pre-marketing clinical trials, drug companies have repeatedly violated the law with impunity: they have failed to include in their submission of data to the FDA, the worst adverse events suffered by subjects who, as a result, dropped out of the trials.

Her observations, published in The American Statesman (below) are disturbing and insightful:

“The study started out with 20 subjects, but 6 were eliminated during the in-patient stay by the drug company sponsoring the trial for various reasons (including drinking caffeine within 24 hours of check-in). For about a week, there were 14 subjects. Then they started dropping. The first one to go was a girl with a pronounced Texas twang named Denise, who had severe jaw and tooth pain. Then extreme nausea and emesis (the clinical term for vomiting, I discovered) claimed April. Jo Kay, Paula, Amy, Alyssa and Carrie went one after another. Now we’re down to 7.”

Ana experienced severe black outs–clearly an adverse effect of the experimental drug–but she was kept in the trial against her best interest:

“The day got off to a bumpy start when I started to black out while reporting my side effects. Darkness closed in from my peripheral vision and then I saw nothing but big colored spots.
“That morning, we were standing around in the cafeteria waiting to dose. All of a sudden, I couldn’t see and lost the ability to balance. If I hadn’t been standing between two of my fellow subjects, who grabbed me and held me up, I would’ve slammed into the floor. I knew I hadn’t fainted; I could still hear just fine, but all I heard was chaos as everyone around me freaked out. I dropped into the nearest chair and put my head between my legs while the study coordinator called the on-site paramedics. While the coordinator frantically called the staff doctor, a paramedic checked and re-checked me. I did fine as long as I wasn’t on my feet for too long. The doctor cleared me to keep dosing.”

Ana explains why her continued “participation” in the trial–disregarding the danger the black outs posed to her well-being–was to accommodate the sponsoring company’s need to maintain a minimum of 7 subjects in the trial:

“The drug company had a dilemma. To submit trial results to the FDA, the study couldn’t fall below seven participants. But, unfortunately, one showed signs of serious side effects and if those results were submitted, approval was highly unlikely. If my results were dropped, the FDA would never know about the problem and the drug company could start fresh with a third trial. However, the first clinical trial had to be scrapped because too many subjects dropped out as a result of their side effects, and it looked like the second study could soon follow the same path. To gather enough healthy volunteers who fit the protocol for a third trial would require a lot of time and money, and it wasn’t something the sponsor was willing to do. So, in the end, my results and I stayed in the study.”

“Because the trial ended with the magic number of seven volunteers, the results could be submitted for review and the FDA had the opportunity to see the data. But what happens in the trials in which drug companies drop some of the subjects with the worst side effects?”

Ana Cantu’s first-hand experience confirms the finding reported by FDA’s safety officer, Dr. Thomas Marciniak, who analyzed the raw data from GSK’s Avandia trial, and found that the company concealed from the FDA the worst adverse event data, resulting in its approval precipitating preventable heart attacks and deaths.

An editorial in today’s New York Times, calls upon the FDA to revoke its questionable approval of Avastin for breast cancer because it failed to extend patients’ lives while it caused serious side effects. The drug had gained “accelerated approval” without adequate testing.

Exactly five years ago, in exchange for the most miserable month of my life, I got paid $4,800 to test the effects of a drug made by GlaxoSmithKline.

You know where you’ve heard the name GlaxoSmithKline recently, right? That’s the company on the verge of losing the approval of the Food and Drug Administration for the diabetes medication Avandia after regulators discovered omissions in a key clinical trial report. On Wednesday, the FDA ordered Glaxo to stop enrolling people in another Avandia trial.

According to a review reassessing the drug’s safety by the FDA’s Dr. Thomas Marciniak, a number of patients taking Avandia appeared to have serious heart problems that were not counted in the study’s tally of adverse events, otherwise known as side effects.

Such repeated mistakes “should not be found even as single occurrences” and “suggest serious flaws with trial conduct,” he wrote.

It can cost hundreds of millions of dollars — in some cases, close to a billion — in research and development for a drug company to secure FDA approval.

By the time a drug gets to point where it can be tested in humans, the pressure for positive results in clinical trials is immense. And I found that out first-hand when as one of the healthy volunteers — a human guinea pig — in a study that tested the effects of Norvir, an HIV drug made by Abbott Laboratories, when coupled with the antidepressant Wellbutrin, made by GlaxoSmithKline.

In exchange for that $4,800 paycheck, I spent about a month going in and out of a blocky silver building in an office park not far from Austin-Bergstrom International Airport, the site of a contract research lab that conducts medical studies.

During the lab’s second clinical trial of the Norvir-Wellbutrin combination, which I chronicled in a personal blog, I was known only subject No. 40.

July 12: I check in tomorrow for 4 days. I’ll be taking an antidepressant and an AIDS drug in combination for about a month.

July 13: The facility is freezing. We’re still waiting on blankets. I should’ve brought a hat and gloves. You can tell the people who do studies regularly by their baggage — they bring extra pillows and blankets and huge rolling suitcases. The building is pretty new and it’s painted in all kinds of “modern” colors like bile, which complement the black-and-white tiled floors nicely. Subjects sleep 8 to a room in bunk beds, though there are only 3 people in my room. …

My first dose of Wellbutrin is tomorrow. I hear it gives you crazy dreams.

July 14: I’ve been stuck so many times today I feel like a junkie. I had to be up by 6:12 a.m. to check vital signs and get a pre-dose blood draw. Then I had breakfast, which I had to finish: two potato, egg and cheese tacos with pico de gallo and a carton of 2% milk, which I don’t like. I took the Wellbutrin at 7:27, so precisely every hour after that I’ve been having blood drawn. For the rest of the day, it’s blood draws only every 2 hours. I carry around a clipboard that has all my procedures and meals scheduled — everything has to be done exactly as it says on the sheet or they can dock pay off your study-completion bonus.

Amusing sign near the toilets: Please do NOT use cellphones in urine monitoring stations.

July 15: Dinner was decent — teriyaki chicken, rice, salad with Italian dressing, a hunk of zucchini bread and a sugar cookie. I tried the cookie and didn’t like the aftertaste so I hid it in a spare napkin and arranged everything else on the tray to conceal it. The cafeteria workers check how much of our food we eat — we’re supposed to finish at least 50% of everything. Sometimes it’s hard, like with yesterday’s trail mix. I hope we get a good snack, which I will take my first bite of at precisely 9:32 p.m.

About half of the subjects have done trials before and say that ours isn’t so bad, even with all the blood draws. Apparently, there are some where you have them every 15 minutes. …The people who usually play Monopoly switched to Uno.

July 23: I started on the AIDS drug on Thursday — 300 mg twice a day. The dosage gets upped to 400 mg tomorrow. I don’t feel bad yet, though I’m sleeping less than normal. And today my stomach objected to the egg facsimile we had to eat.

July 25: I was pretty excited that I didn’t get sick after my dosings. … I think the secret is to not drink the milk. And not to eat more than 50% of the food. I’m becoming an expert in artfully rearranging things on my plate so it looks like I’ve eaten. They (try to) make us eat after taking the giant AIDS pills, but since we get the same few meals over and over, it’s gotten really hard to do. Plus, there’s a chance you’ll get sick after so you really don’t want to see nasty food twice, if you get my meaning.

July 28: I discovered that I feel better if I don’t eat after taking the horse pills. This morning, I refused to eat the breakfast tacos and felt fine. So I followed the same strategy at dinner — I did eat the peas and carrots and drank some caffeine-free root beer, but most of the meal was untouched.

Over the course of the trial, as a result of a near-constant state of nausea, I lost about 10 percent of my body weight.

To keep up my strength, for lunch, I’d go to a fast-food restaurant and order the heaviest combo on the menu (double bacon cheeseburger, fries and a huge non-caffeinated beverage) and eat as much as I could before I started to feel sick again.

Every night, insomnia cut my sleep to three hours.

Aug. 1: The study started out with 20 subjects, but 6 were eliminated during the in-patient stay by the drug company sponsoring the trial for various reasons (including drinking caffeine within 24 hours of check-in). For about a week, there were 14 subjects. Then they started dropping. The first one to go was a girl with a pronounced Texas twang named Denise, who had severe jaw and tooth pain. Then extreme nausea and emesis (the clinical term for vomiting, I discovered) claimed April. Jo Kay, Paula, Amy, Alyssa and Carrie went one after another. Now we’re down to 7. In what I view as biological injustice, none of the males have shown noticeable symptoms.

Aug. 2: I had to go see an opthamologist today, just for my safety, since I reported a migraine with aura a few days ago. Unfortunately, I’m fine. Curses. I was hoping I could get medically excused from the study — that way I’d still get paid. But it looks like I’m going to have to finish it. Only 10 more days of dosing to go. My current side effects include oral numbness and tingling in my extremities.

Aug. 6: It’s another day in lockup: cloudy skies (I think) and cold air conditioning. The day got off to a bumpy start when I started to black out while reporting my side effects. Darkness closed in from my peripheral vision and then I saw nothing but big colored spots.

That morning, we were standing around in the cafeteria waiting to dose. All of a sudden, I couldn’t see and lost the ability to balance. If I hadn’t been standing between two of my fellow subjects, who grabbed me and held me up, I would’ve slammed into the floor. I knew I hadn’t fainted; I could still hear just fine, but all I heard was chaos as everyone around me freaked out. I dropped into the nearest chair and put my head between my legs while the study coordinator called the on-site paramedics. While the coordinator frantically called the staff doctor, a paramedic checked and re-checked me. I did fine as long as I wasn’t on my feet for too long. The doctor cleared me to keep dosing.

A few days after my first blackout episode, during a scheduled outpatient visit, one of the study coordinators said I had to be examined by the on-staff doctor. “Why?” “The sponsor is concerned about your side effects,” she said.

The drug company had a dilemma. To submit trial results to the FDA, the study couldn’t fall below seven participants. But, unfortunately, one showed signs of serious side effects and if those results were submitted, approval was highly unlikely. If my results were dropped, the FDA would never know about the problem and the drug company could start fresh with a third trial. However, the first clinical trial had to be scrapped because too many subjects dropped out as a result of their side effects, and it looked like the second study could soon follow the same path. To gather enough healthy volunteers who fit the protocol for a third trial would require a lot of time and money, and it wasn’t something the sponsor was willing to do. So, in the end, my results and I stayed in the study.

Aug. 21: So yesterday I had the exit screening/physical for my drug study. I had to have my blood pressure checked 3 times because it was low, even for me. The paramedic checked me, but I was asymptomatic. She asked how I was feeling. “Fine, especially now that I’m off the drugs.” She said, “Well, it was for the good of mankind.” “I guess … and the money.”

Because the trial ended with the magic number of seven volunteers, the results could be submitted for review and the FDA had the opportunity to see the data. But what happens in the trials in which drug companies drop some of the subjects with the worst side effects?

Actually, we’ve seen what happens — with Avandia.

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When a Drug Fails
THE NEW YORK TIMES July 25, 2010

The flameout of an enormously expensive drug to treat advanced breast cancer will pose a critical test for the Food and Drug Administration. Will the agency have the courage to reverse course when a medical treatment that it approved based on preliminary evidence flops badly in follow-up studies?

Two years ago, the F.D.A. gave Avastin, which is made by the Genentech unit of Roche, “accelerated approval” as a treatment for breast cancers that have spread to other parts of the body. Such cancers are essentially incurable so the best that current treatments can do is extend a patient’s life.

The hurry-up mechanism allows approval of a drug that has not yet been proved safe and effective in thorough clinical trials but has shown promise that it might benefit patients with life-threatening diseases. Rather than make such patients wait, they are treated with the drug while the manufacturer completes additional tests.

When Avastin was granted “accelerated approval” to treat advanced breast cancer, the primary evidence was a single clinical trial. It found that Avastin, when used with another drug, slowed progression of the disease but did not significantly extend patients’ lives.

Now two follow-up trials by the manufacturer have failed to confirm even those meager gains. In the initial trial, Avastin held tumor progression at bay for five and a half months. In the two new trials, pairing Avastin with different chemotherapy drugs, the delay in tumor worsening was much shorter: up to three months in one trial and less than a month in the other. The Avastin combinations also caused serious side effects.

Britain’s National Institute for Health and Clinical Excellence, a pace-setter in evaluating medical advances, issued draft guidance this month against using Avastin for advanced breast cancer patients in the National Health Service. It called the clinical trial data “disappointing” and the cost “too high for the limited and uncertain benefit it may offer patients.”

By a 12-to-1 vote last week, an F.D.A. advisory committee quite sensibly urged the agency to revoke Avastin’s approval for breast cancer. That would not affect its other approvals, gained through the standard regulatory process, for treating colon, lung, kidney and brain cancers. Avastin would remain available to doctors for off-label use against breast cancer. Many insurers, however, might refuse to cover an unapproved use.

The cost of Avastin has always seemed outrageously high for the medical benefits it confers. The wholesale price for a typical breast cancer patient is about $88,000 a year. Genentech has been capping annual spending at $57,000 for patients with incomes below $100,000.

The F.D.A. has rarely removed drugs that were given accelerated approval and sometimes has failed even to compel completion of follow-up studies. But there are signs it may get tougher. In June, the agency finally forced a leukemia drug off the market that had been given accelerated approval a decade ago, after a long- delayed follow-up study showed no clinical benefit and an increased risk of death. With Avastin, the follow-up studies were completed in a timely manner — with such meager results that withdrawal seems the right response.

Just Exactly What Do Dr. Rima and Gen. Bert DO At Codex?
Find Out About Our Next Guest on the Dr. Rima Reports
Four Blog Links You MUST Click!
On the Road to Codex
Current ‘Must Take’ Action Items
Dr.Rima Recommends

Your generosity and support sends Natural Solutions Foundation to a variety of Codex meetings around the world. Right now General Bert and I are in Geneva Switzerland. We left our home at the Valley of the Moon Eco Demonstration Project in Volcan, Panama, www.NaturalSolutionsFoundation.org, to get on a plane to Panama City, then another one to Madrid and another one to Genva two days ago so that by the time we reached Switzerland we had not slept for about 48 hours. Why didn’t we take a quicker, more direct route? Because neither General Stubblebine nor I am willing to expose our bodies to the radiation hazard of full body scanners and neither Madrid nor Geneva airports use full body scanners.

We got to Geneva and continued our preparation for the meeting. You see, in order bring you intelligent, meaningful and precise information in our daily video and written reports and later create meaningful strategies to deal with Codex and its dangers, we need to do a major amount of planning and preparation.

Codex is designed to be overwhelmingly complex, detail driven and difficult to comprehend because the technical level of the considerations is so enormously demanding if you are going to understand it all. Delegates are just supposed to be so overwhelmed that they simply sink into a lulled position in which whatever the US or EU says is what they go along with, sort of like the courtiers just letting the red queen do what she likes in Alice and Wonderland because it is so much easier and safer.

But at Codex, as in so many other urgently important situations, the devil really IS in the details. Consider:

There are 15 Committee Reports to be studied from major codex Committees (http://www.codexalimentarius.net/web/archives.jsp) for the Codex Alimentarius Commission (CAC) session starting on Monday, July 5.

The Report of the Codex Executive Committee has 28 pages

The Committee on Food Labeling has 58 pages

The Committee on Contaminants in Foods has 69 pages

and so on through the 15 committees presenting their items for discussion at the CAC.

Potentially buried in each one of the clauses, phrases, reports and agenda items is a time bomb that can, despite its innocuous language, kill people through the implications and permissions granted via its legalese.

Nutrient Reference Values (NRVs) and GMO labeling are excellent, but by no means unique, examples. Both of these issues are highly technical and both, if carried out as the US desires, would lead to highly undesirable outcomes. NRVs are daily intake values of nutrients so low that they actually introduce and make permanent, the under-nutrition which WHO and FAO point out as the primary cause of the non-communicable, preventable, degenerative killer diseases: cancer, cardiovascular disease, stroke, diabetes and obesity. Misleading consumers into believing that their processed food provides adequate levels of vital nutrients, the NRVs are both a biochemical absurdity and an atrocity since they will, through their use on labels, lead people to believe that since their food is providing most or all of the NRVs, it provides the nutrients they need for a healthy life.

NRVs have been winding their way through the Codex Committee on Nutrition and Foods for Special Dietary Uses (CCNFSDU) and the Committee on Food Labeling (CCFL). When South Africa was discussing them in 2005 at CCNFSDU, Dr. Grossklaus, the Chairman cut the delegate off at the knees when she mentioned “optimal nutrition” and said “It would be nice if Codex were about nutrition, but it isn’t. It’s about trade!” But most delegates have no idea what biochemical individuality is about, why high potency nutrients save lives, money and misery and the discussions must include the technical issues of the Codex texts and committee which are dealing with NRVs, their status in the CAC, etc. To learn more about where this nutrients as toxins, nutrients as controlled substances, idea in Codex, click here to watch “Nutricide”: http://video.google.com/videoplay?docid=-5266884912495233634#.

GMO labeling is another example, as is whether Codex should define consensus or a code of ethics for codex participants. In these discussions and decisions, information lies which could, going in one direction, change history and survival for good and, going in the other direction, could do exactly the opposite.

Each Agenda Item rests on a multi-year background with a huge pile of data and debate behind it. Having that perspective is essential to informed, effective dialogue with the delegates at Codex and in their home countries. And that is what we do at Codex! We take your interests, and those of well-nourished, autonomous, food independent people and “bang them against” what Codex is doing. The lives of food producers, food consumers and the planet turn on these tiny nuances since all of the Codex documents are written in such a way as to lull you into a fluorided haze of complacency. There is, however, nothing to be complacent about.

There is also nothing worth participating in at Codex. It is my contention that the United States needs to get out of Codex and do it now. We will lose nothing and grain a great deal, I believe, by loosening the hold that we have allowed the World Trade Organization, WHO, to place on us through trade agreements that can only inevitably degrade our food and our health unless we follow the Codex Two Step Process, as other nations have done successfully. If we were out of Codex, I believe that two things would happen:

First, it would be a great deal easier for interested parties to apply pressure to force the US to deviate from the Codex guidelines and standards since we would not have teams of experts ramming these guidelines and standards through Codex and, second, we would not be twisting and distorting the entire Codex process, making the decisions that the US wants, not the ones that protect the farmers, the consumers and the earth. By the way, the Developed World is one of the major consumers of third world-produced toxic food. Here is the link to my video:

There are at least a hundred equally vital items before the CAC this week. They would be far better decided by the national competencies of the countries rather than by the “bully of the class” threatening the other kids in the class with the active and vigorous help of the corrupt and self interested “teacher”, WHO, a corrupt and genocidal organization which acknowledges that it wants to see the population of the earth reduced by a minimum of 80%, better 90%!

So what we do is prepare for the topics of greatest interest to you and to the developing world’s delegates, mingle with delegates and share our perspectives on these topics and provide leadership for dissent strategies. Then, very importantly, we offer them information on how they can increase crop yield, decrease food born illness, and, in reality, actually accomplish exactly what Codex says it is about.

And we report. After each day’s meetings, we make sure that you know what the highlights (and low points) of the day’s proceedings have been, what they mean for you, what they mean for the dangerous forward movement of “HARMonization” by the US and how to protect ourselves, our health and our health freedom.

Attending Codex is really hard work. We do it for you, with your support because it is hugely important. At the end of a Codex meeting we are exhausted. Then we fly home to Panama to put the things we are teaching the developing world into practice.

Our Natural Solutions Center will be opening at the Valley of the Moon™ Eco Demonstration Project in Volcan, Panama, on August 7/8, 2010. You are invited. Please join us for this important step forward. You can see the health protocols that we plan to offer if you visit www.DrRima.net. And you can be with us for the initiation of what is, in essence, the exact opposite of what Codex is about. We’ll be living, teaching, sharing and creating clean food and vital freedom through education and dissemination, demonstration and direction.

For more information on the Valley of the Moon™ Eco Demonstration Project, how you can participate in it, live there, work there, safeguard your retirement income there and otherwise be a huge part of this innovative freedom project, please visit www.NaturalSolutionsFoundation.org. And if you would like to join our very active NSF-Panama Forum on Yahoo.com, please visit http://tech.groups.yahoo.com/group/NSF-Panama/join to become part of this vital community while you still can.

And, oh, yes, don’t forget that the limited supply of our amazing Valley of the Moon™ Coffee is available for you now. If you want premium Panamanian Highland coffee grown without a single chemical contaminant, you need to place your order before it is all gone. Don’t forget your corporate gifts this holiday season and your personal ones. Order now and we will make sure that your recipients are not left out in the gift-giving cold this year! Make your tax deductible donation and get what we believe you will agree is the best coffee you have ever tasted at www.ValleyoftheMoonCoffee.org.

Because of high winds, we had to cut down 80% of our plants to allow them to regrow so this scarce beauty of a coffee is even scarcer. Our harvest is magnificent, but the best coffee in the world, and the cleanest, is even more rare than last year! We have not raised the price of a donation, but make sure you get as much as you need before there is no more left this year.

And, as hard as it is, thanks for sending us to Codex. We still need your donations to finish defraying the cost (Geneva, Switzerland is a very expensive place!)

1. 9 PM: Dr. Rima and Co-Host Ralph Fuectola address this week’s health freedom news and rumors — We’ll discuss the heath freedom information and sort out the disinformation for you…including
What to Expect from the Codex Meeting in Geneva…

The Valley of the Moon™ Eco Demonstration Project’s Natural Solutions Institute, which we call the “Dr. Rima Institute” for short, is about to open in the beautiful, bountiful, temperate highlands community of Volcan, Panama on August 7-8, 2010 and you are invited!

You can read more about this long-awaited opening, follow our progress (we will be posting photos and videos!) at the Dr. Rima Network web site:www.DrRima.net where you will also find a description of many of the natural protocols to be offered at the Institute and some of the products we love

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Valley of the Moon™ BeyondOrganic Coffee

Supplies are Limited for this Artisenal, Hand Picked and Roasted Coffee. Place your gift orders now for yourself and friends.

Valley of the Moon™ Coffee make a wonderful corporate gift for friends, colleagues and clients. Gifts say a lot about the giver. Your impeccable taste is revealed when you give GMO-Free, Toxin-Free, Non Toxic Valley of the Moon™ Coffee This Year!

Health Freedom’s Own Coffee, Valley of the Moon Coffee, Will Delight You, While You Support the Natural Solutions Foundation With Your Morning Java! Make a donation and get your coffee. Once you taste this exceptional brew, we know you will love it! Write to us at dr.laibow@gmail.com to let us know your experience drinking Valley of the Moon Coffee. We are confident that it will the finest cup of coffee you have ever tasted in your life, bar none!

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Cognitive Enhancement Nutrition: Empower Your Mind!

Dr. Rima and Gen. Bert love these leading-edge products… Control your own mind! Feed your brain what it needs for discernment and acuity… “These are the times that try men’s souls…” Are you ready?

Dr. Rima has designed a third, very special Dietary Supplement Mind Enhancement Pack!
To learn more, or to try the products, go to:
Cognitive Enhancement“News & Specials” lista the three Dr. Rima Packs For more Details about the Packs:
http://drrimatruthreports.com/?p=4558

You know there is a battle going on for your mind (or maybe against it!). Part of the Globalist Agenda to reduce human population and restrict our freedoms goes on in our own heads, as we are subjected to a level of propaganda that can only be termed “mind controlling.” Its success depends on making sure that we are dumb, dull, deluded and distracted….

Let me quote General Bert, “‘Focus and clarity’ were the words Ralph used to describe the Cognitive Enhancement nutrients, and that is exactly what I experienced. Both my long and short term memory are enhanced by these products and my thinking processes are noticeably sharper. I am very impressed and intend to continue using them.”

There are numerous smart nutrients, but few of them, working synergistically, have the capability of doing what these products actually do. In this battle to take back our food, our health and our freedoms, we must all be as mentally sharp as possible. That is why the genocidal elitists want us under-nourished and unable to think. I was so impressed with these products that I immediately began to study them and their impact. I researched the ingredients and am satisfied that there is no indication of a lack safety when used as directed. That’s when I decided to create combination packs that would support mental function without agitating; would enhance cognition without later let-down. Dr. Rima

If you’ve had problems placing orders for these extraordinary nutrients, we’ve set up a special email address for you to use; just email your contact information and we’ll have you called back right away!
brians@biologicsnutra.com

Natural Solutions Foundation has no corporate sponsorship. YOU are our only sponsors, but the goods and services come from companies who believe in what we are doing. Every sale helps to support the Foundation and move our health freedom actions forward. We urge you to patronize these mission-driven malls where you will find outstanding ways to support and be supported as free men and women!